Short-acting benzodiazepine salts and their polymorphic forms

ABSTRACT

The invention relates to besylate salts of the compound of formula (I): 
     
       
         
         
             
             
         
       
     
     Methods of preparing the salts, and their use as medicaments, in particular for sedative or hypnotic, anxiolytic, muscle relaxant, or anticonvulsant purposes is also described.

CROSS-REFERENCES TO RELATED APPLICATIONS

This application is a continuation of currently pending U.S. applicationSer. No. 15/908,081, filed Feb. 28, 2018 which is a continuation of U.S.Pat. No. 9,914,738 issued Mar. 13, 2018 (U.S. application Ser. No.15/703,945, filed Sep. 13, 2017), which is a continuation of U.S. Pat.No. 9,777,007 issued Oct. 3, 2017 (U.S. application Ser. No. 14/948,889,filed Nov. 23, 2015), which is a continuation of U.S. Pat. No. 9,193,730issued Nov. 24, 2015 (U.S. application Ser. No. 12/373,472, filed Nov.2, 2009), which is the U.S. National Stage of International ApplicationNo. PCT/GB2007/002565, filed Jul. 10, 2007, which designated the UnitedStates and has been published as International Publication No. WO2008/007071 and which claims the priority of Great Britain PatentApplications, Serial Nos.: 0613694.9 and 0613692.3 of Jul. 10, 2006,pursuant to 35 U.S.C. 119(a)-(d). The contents of the aforementionedapplications are hereby incorporated herein by reference.

BACKGROUND OF THE INVENTION

This invention relates to salts of a short acting benzodiazepine, and touse of the salts as medicaments, in particular for sedative or hypnotic,anxiolytic, muscle relaxant, or anticonvulsant purposes.

European Patent No. 1,183,243 describes short-acting benzodiazepinesthat include a carboxylic acid ester moiety and are inactivated bynon-specific tissue esterases. An organ-independent eliminationmechanism is predicted to be characteristic of these benzodiazepines,providing a more predictable and reproducible pharmacodynamic profile.The compounds are suitable for therapeutic purposes, includingsedative-hypnotic, anxiolytic, muscle relaxant and anticonvulsantpurposes. The compounds are short-acting CNS depressants that are usefulto be administered intravenously in the following clinical settings:preoperative sedation, anxiolysis, and amnestic use for perioperativeevents; conscious sedation during short diagnostic, operative orendoscopic procedures; as a component for the induction and maintenanceof general anesthesia, prior and/or concomitant to the administration ofother anaesthetic or analgesic agents; ICU sedation.

One of the compounds disclosed in EP 1,183,243 (in Example Ic-8, page36) is Methyl 3-[(4S)-8-bromo-1-methyl-6-(2-pyridinyl)-4H-imidazol[1,2-a] [1,4]benzodiazepin-4-yl] propanoate, as shown in formula (I)below:

Whilst the free base of formula (I) is stable when stored at 5° C.,samples stored at 40° C./75% relative humidity (open) are observed todeliquesce, become yellow to orange in colour, and show notabledecreases in content relative to initial (see Example 1 below).

It has now surprisingly been found that the compound of formula (I)forms highly crystalline mono (benzenesulfonic acid) besylate salts thatare easily isolated from a range of pharmaceutically acceptable solventsand show good thermal stability, low hygroscopicity and high aqueoussolubility.

SUMMARY OF THE INVENTION

According to the invention there is provided a besylate salt of acompound of formula (I). Preferably the salt is a crystalline salt.Preferably the crystalline salt has a stoichiometry of 1:1 compound offormula (I):besylate. Preparation and characterisation of polymorphicforms of besylate salts is described in the Examples below.

According to the invention there is provided a crystalline polymorph ofa besylate salt of a compound of formula (I) (herein designated besylateForm 1), that exhibits an X-ray powder diffraction (XRPD) pattern whichcomprises a characteristic peak at about 7.3, 7.8, 9.4, 12.1, 14.1,14.4, 14.7, or 15.6 degrees two-theta.

Preferably the besylate Form 1 crystalline polymorph exhibits an XRPDpattern which comprises characteristic peaks at about 7.3, 7.8, 9.4,12.1, 14.1, 14.4, 14.7, and 15.6 degrees two-theta.

More preferably the besylate Form 1 crystalline polymorph exhibits anXRPD pattern which comprises characteristic peaks at: 7.25 (10.60), 7.84(72.60), 9.36 (12.10), 12.13 (32.50), 14.06 (48.50), 14.41 (74.30),14.70 (50.70), 15.60 (26.90) [angle two-theta degrees (percentagerelative intensity)].

Preferably the besylate Form 1 crystalline polymorph has a differentialscanning calorimetry (DSC) onset melting temperature in the range187-204° C., preferably about 191-192° C.

A crystal structure of Form 1 has been resolved at 190K (R factor of6.3). Form I has a stoichiometry of 1:1 compound:besylate. Itscrystallographic asymmetric unit contains two independent compoundmolecules and two besylate molecules. The two independent compoundmolecules are singly protonated on the imidazole ring. The crystalstructure has unit cell dimensions of a=7.6868 Å, b=29.2607 Å, c=12.3756Å, α=90°, β=97.7880°, γ=90°, and a space group of P2₁. The crystalstructure is described in more detail in Example 9, and crystallographiccoordinates are given in Table 17. Bond lengths and angles for Form 1are given in Tables 19 and 20, respectively.

According to the invention there is provided a besylate salt of acompound of formula (I) which is a crystalline polymorph comprising acrystal with unit cell dimensions of a=7.6868 Å, b=29.2607 Å, c=12.3756Å, α=90°, β=97.7880°, γ=90°.

There is also provided according to the invention a besylate salt of acompound of formula (I) which is a crystalline polymorph having acrystal structure defined by the structural coordinates as shown inTable 17.

There is further provided according to the invention a besylate salt ofa compound of formula (I) with bond lengths and angles as shown inTables 19 and 20, respectively.

There is further provided according to the invention a crystallinepolymorph of a besylate salt of a compound of formula (I) (hereindesignated besylate Form 2), that exhibits an XRPD pattern whichcomprises a characteristic peak at about 8.6, 10.5, 12.0, 13.1, 14.4, or15.9 degrees two-theta.

Preferably the besylate Form 2 crystalline polymorph exhibits an XRPDpattern which comprises characteristic peaks at about 8.6, 10.5, 12.0,13.1, 14.4, and 15.9 degrees two-theta.

More preferably the besylate Form 2 crystalline polymorph exhibits anXRPD pattern which comprises characteristic peaks at: 8.64 (17.60),10.46 (21.00), 12.03 (22.80), 13.14 (27.70), 14.42 (11.20), 15.91(100.00) [angle two-theta degrees (percentage relative intensity)].

Preferably the besylate Form 2 crystalline polymorph has a differentialscanning calorimetry (DSC) onset melting temperature in the range170-200° C., preferably about 180° C.

A crystal structure of Form 2 has been resolved at 190K (R factor of3.8). Form 2 has stoichiometry of 1:1 compound:besylate. Itscrystallographic asymmetric unit contains one compound molecule and onebesylate molecule. The compound molecule is singly protonated on theimidazole ring. The crystal structure has unit cell dimensions ofa=8.92130 Å, b=11.1536 Å, c=25.8345 Å, α=90°, β=90°, γ=90°, and a spacegroup of P2₁2₁2₁. The crystal structure is described in more detail inExample 10, and crystallographic coordinates are given in Table 18. Bondlengths and angles for Form 2 are given in Tables 21 and 22,respectively.

According to the invention there is provided a besylate salt of acompound of formula (I) which is a crystalline polymorph comprising acrystal with unit cell dimensions of a=8.92130 Å, b=11.1536 Å, c=25.8345Å, α=90°, β=90°, γ=90°.

There is also provided according to the invention a besylate salt of acompound of formula (I) which is a crystalline polymorph having acrystal structure defined by the structural coordinates as shown inTable 18.

There is further provided according to the invention a besylate salt ofa compound of formula (I) with bond lengths and angles as shown inTables 21 and 22, respectively.

There is further provided according to the invention a crystallinepolymorph of a besylate salt of a compound of formula (I) (hereindesignated besylate Form 3), that exhibits an X-ray powder diffraction(XRPD) pattern which comprises a characteristic peak at about 7.6, 11.2,12.4, 14.6, 15.2, 16.4, or 17.7 degrees two-theta.

Preferably the besylate Form 3 crystalline polymorph exhibits an XRPDpattern which comprises characteristic peaks at about: 7.6, 11.2, 12.4,14.6, 15.2, 16.4, and 17.7 degrees two-theta.

More preferably the besylate Form 3 crystalline polymorph exhibits anXRPD pattern which comprises characteristic peaks at: 7.61 (65.70),11.19 (33.20), 12.38 (48.70), 14.63 (30.60), 15.18 (33.20), 16.40(29.60), 17.68 (51.30) [angle 2θ° (percentage relative intensity)].

Preferably the besylate Form 3 crystalline polymorph has a differentialscanning calorimetry (DSC) onset melting temperature in the range195-205° C., preferably about 200-201° C.

There is further provided according to the invention a crystallinepolymorph of a besylate salt of a compound of formula (I) (hereindesignated besylate Form 4), that exhibits an XRPD pattern whichcomprises a characteristic peak at about 7.6, 10.8, 15.2, 15.9, or 22.0degrees two-theta.

Preferably the besylate Form 4 crystalline polymorph exhibits an XRPDpattern which comprises characteristic peaks at about: 7.6, 10.8, 15.2,15.9, and 22.0 degrees two-theta.

Preferably the besylate Form 4 crystalline polymorph exhibits an XRPDpattern which comprises characteristic peaks at: 7.62 (83.50), 10.75(14.70), 15.17 (37.80), 15.85 (28.70), 22.03 (100) [angle 2θ°(percentage relative intensity)].

Preferably the besylate Form 4 crystalline polymorph has a differentialscanning calorimetry (DSC) onset melting temperature in the range180-185° C., preferably about 182° C.

A preferred salt is the besylate Form 1 based on the robustness offormation, yield, purity and chemical and solid form stability.

There is also provided according to the invention a method of making abesylate salt of a compound of formula (I), which comprises reacting afree base of a compound of formula (I) with benzene sulfonic acid.

Also according to the invention there is provided a method of making asalt of the invention, which comprises contacting a free base of acompound of formula (I) with benzene sulfonic acid in solution to causeformation of a precipitate of the besylate salt. Preferably the methodfurther comprises isolating the precipitate.

Preferably the free base is dissolved in toluene, ethanol, ethylacetate, MtBE, dichloromethane (DCM), isopropyl acetate, ethyl formate,methanol, or acetone. More preferably the free base is dissolved intoluene or ethyl acetate. Preferably the benzene sulfonic acid isdissolved in ethanol.

The besylate Form 1 may be prepared by contacting a solution of a freebase of a compound of formula (I) in toluene, ethyl acetate, acetone,isopropyl acetate, or ethyl formate with a solution of benzene sulfonicacid in ethanol to cause formation of a precipitate of the salt.

There is also provided according to the invention a besylate salt of acompound of formula (I) which is obtainable by the above method.

The besylate Form 2 may be prepared by contacting a solution of a freebase of a compound of formula (I) in methanol with a solution of benzenesulfonic acid in ethanol to cause formation of a precipitate of thesalt. Preferably the mixture is cooled below ambient temperature (forexample 4° C.).

There is also provided according to the invention a besylate salt of acompound of formula (I) which is obtainable by the above method.

The besylate Form 3 may be prepared by seeding liquor resulting fromcrystallisation of Form 1 from ethyl acetate/ethanol with Form 1.Preferably the liquor is cooled below ambient temperature (for example4° C.).

In one embodiment the besylate Form 3 may be prepared by seeding, with abesylate Form 1 crystalline salt of a compound of formula (I), afiltrate solution separated from the precipitate formed by contacting asolution of a compound of formula (I) in ethyl acetate with a solutionof benzene sulfonic acid in ethanol, to produce the besylate Form 3crystalline polymorph.

There is also provided according to the invention a besylate salt of acompound of formula (I) which is obtainable by any of the above methods.

The besylate Form 4 may be prepared by re-crystallising besylate Form 1from isopropyl acetate/ethanol, preferably 40% isopropylacetate/ethanol.

There is also provided according to the invention a besylate salt of acompound of formula (I) which is obtainable by the above method.

Salts of the invention may also be prepared by crystallising compound offormula (I) besylate from a suitable solvent, or from a suitablesolvent/anti-solvent or solvent/co-solvent mixture. The solution ormixture may be cooled and/or evaporated to achieve crystallisation ifappropriate.

We have found that crystallisation of Form 2 is observed in conditionswhere there are extremes of either polarity (for exampleacetonitrile:water) or lipophilicity (n-nonane), or both (dimethylsulfoxide:1,2-dichlorobenzene).

Examples of solvents for crystallisation of Form 2 are: nonane;methanol.

Examples of solvent/anti-solvent mixtures for crystallisation of Form 1are: dimethylacetamide/methyl isobutyl ketone;dimethylacetamide/tetrachloroethylene; acetonitrile/3-methylbutan-1-ol;acetonitrile/1,2-dichlorobenzene; acetonitrile/pentylacetate;methanol/3-methylbutan-1-ol; methanol/methyl isobutyl ketone;2,2,2-trifluoroethanol/1,4-dimethylbenzene; ethanol/methyl isobutylketone; ethanol/1,4-dimethylbenzene; propan-1-ol/1,2-dichlorobenzene;propan-1-ol/tetrachloroethylene; propan-2-ol/1,2-dichlorobenzene;propan-2-ol/n-nonane; 2-methoxy ethanol/water; 2-methoxy ethanol/pentylacetate; 2-methoxy ethanol/1,4-dimethylbenzene; tetrahydrofuran/water;tetrahydrofuran/3-methylbutan-1-ol; tetrahydrofuran/1,2-dichlorobenzene;tetrahydrofuran/ethyl acetate; tetrahydrofuran/1,3-dimethylbenzene.

Examples of solvent/anti-solvent mixtures for crystallisation of Form 2are: ethanol/ethyl acetate; ethanol/methyl isobutyl ketone;ethanol/p-cymene; dimethylsulfoxide/1,2-dichlorobenzene;acetonitrile/water; ethano/1,2-dichlorobenzene;ethanol/tetrachloroethylene; tetrahydrofuran/1,2-dichlorobenzene;tetrahydrofuran/ethyl acetate.

According to a preferred embodiment, Form 1 is crystallised from2-methoxyethanol/pentyl acetate.

According to a preferred embodiment, Form 2 is crystallised fromethanol/ethyl acetate.

According to a preferred embodiment, Form 2 is crystallised frommethanol/ethanol (preferably by cooling a solution of compound offormula (I) besylate in methanol/ethanol below ambient temperature, forexample 4° C.).

According to a preferred embodiment, Form 3 is crystallised fromethanol/ethyl acetate (suitably by cooling the mixture below ambienttemperature, for example 4° C.).

According to a preferred embodiment, Form 4 is crystallised fromisopropyl acetate/ethanol (preferably by cooling a solution of compoundof formula (I) besylate in isopropyl acetate/ethanol to ambienttemperature).

There is also provided according to the invention a besylate salt of acompound of formula (I) obtainable by any of the above methods.

Methods of preparing salts of the invention are described in detail inthe Examples below.

A salt of the invention may be used as a medicament, in particular forsedative or hypnotic, anxiolytic, muscle relaxant, or anticonvulsantpurposes.

While it is possible for a salt of the invention to be administered as abulk active chemical, it is preferably provided with a pharmaceuticallyacceptable carrier, excipient, or diluent in the form a pharmaceuticalcomposition. The carrier, excipient, or diluent must, of course, beacceptable in the sense of being compatible with the other ingredientsof the composition and must not be deleterious to the recipient.

Accordingly, the present invention provides a pharmaceutical compositioncomprising a salt of the invention and a pharmaceutically acceptablecarrier, excipient, or diluent.

Pharmaceutical compositions of the invention include those suitable fororal, rectal, topical, buccal (e.g. sub-lingual) and parenteral (e.g.subcutaneous, intramuscular, intradermal or intravenous) administration.

Preferably a salt of the invention is provided in the form of apharmaceutical composition for parenteral administration, for example,by intravenous or intramuscular injection of a solution. Where thepharmaceutical composition is for parenteral administration, thecomposition may be an aqueous or non-aqueous solution or a mixture ofliquids, which may include bacteriostatic agents, antioxidants, buffersor other pharmaceutically acceptable additives.

A preferred formulation of a salt of the invention is in an aqueousacidic medium of pH 2-4 or in an aqueous solution of a cyclodextrin(CD). Cyclodextrins that can be used for these formulations are eitherthe anionically charged sulfobutylether (SBE) derivatives of β-CD,specifically SBE7-β-CD, marketed under the tradename Captisol by CyDex,Inc. (Critical Reviews in Therapeutic Drug Carrier Systems, 14 (1),1-104 (1997)), or the hydroxypropyl CD's.

A further preferred formulation of a salt of the invention is alyophilised formulation comprising, in addition to the salt, at leastone of the following agents: ascorbic acid, citric acid, maleic acid,phosphoric acid, glycine, glycine hydrochloride, succinic acid ortartaric acid. These agents are believed to be useful as buffering,caking or vizualisation agents. In some cases it may be beneficial toinclude sodium chloride, mannitol, polyvinylpyrrolidone, or otheringredients in the formulation.

The preferred method of formulation (i.e., acid buffer or CD-based) maydepend on the physicochemical properties (e.g., aqueous solubility, pKa,etc.) of a particular salt. Alternatively the salt may be presented as alyophilized solid for reconstitution with water (for injection) or adextrose or saline solution. Such formulations are normally presented inunit dosage forms such as ampoules or disposable injection devices. Theymay also be presented in multi-dose forms such as a bottle from whichthe appropriate dose may be withdrawn. All such formulations should besterile.

According to the invention there is provided a method for producingsedation or hypnosis in a subject, which comprises administering aneffective sedative or hypnotic amount of a salt of the invention to thesubject.

There is also provided according to the invention a method for inducinganxiolysis in a subject, which comprises administering an effectiveanxiolytic amount of a salt of the invention to the subject.

There is further provided according to the invention a method forinducing muscle relaxation in a subject, which comprises administeringan effective muscle relaxant amount of a salt of the invention to thesubject.

There is further provided according to the invention a method fortreating convulsions in a subject, which comprises administering aneffective anticonvulsant amount of a salt of the invention to thesubject.

According to the invention there is also provided use of a sedative orhypnotic amount of a salt of the invention in the manufacture of amedicament for producing sedation or hypnosis in a subject.

According to the invention there is also provided a salt of theinvention for producing sedation or hypnosis in a subject.

There is also provided according to the invention use of an anxiolyticamount of a salt of the invention in the manufacture of a medicament forproducing anxiolysis in a subject.

There is also provided according to the invention a salt of theinvention for producing anxiolysis in a subject.

There is further provided according to the invention use of a musclerelaxant amount of a salt of the invention in the manufacture of amedicament for producing muscle relaxation in a subject.

There is further provided according to the invention a salt of theinvention for producing muscle relaxation in a subject.

There is further provided according to the invention use of ananticonvulsant amount of a salt of the invention in the manufacture of amedicament for treating convulsions in a subject.

There is further provided according to the invention a salt of theinvention for treating convulsions in a subject.

The subject is suitably a mammal, preferably a human.

A suitable pharmaceutical parenteral preparation for administration tohumans will preferably contain 0.1 to 20 mg/ml of a salt of theinvention in solution or multiples thereof for multi-dose vials.

Intravenous administration can take the form of bolus injection or, moreappropriately, continuous infusion. The dosage for each subject mayvary, however, a suitable intravenous amount or dosage of a salt of theinvention to obtain sedation or hypnosis in a mammal would be 0.01 to5.0 mg/kg of body weight, and more particularly, 0.02 to 0.5 mg/kg ofbody weight, the above being based on the weight of the salt which isthe active ingredient. A suitable intravenous amount or dosage of a saltof the invention to obtain anxiolysis in a mammal would be 0.01 to 5.0mg/kg of body weight, and more particularly, 0.02 to 0.5 mg/kg of bodyweight, the above being based on the weight of the salt which is theactive ingredient. A suitable intravenous amount or dosage of a salt ofthe invention to obtain muscle relaxation in a mammal would be 0.01 to5.0 mg/kg of body weight, and more particularly, 0.02 to 0.5 mg/kg ofbody weight, the above being based on the weight of the salt which isthe active ingredient. A suitable intravenous amount or dosage of a saltof the invention to treat convulsions in a mammal would be 0.01 to 5.0mg/kg of body weight, and more particularly, 0.02 to 0.5 mg/kg of bodyweight, the above being based on the weight of the salt which is theactive ingredient.

Salts of the invention are short-acting CNS depressants that are usefulto be administered intravenously in the following clinical settings:preoperative sedation, anxiolysis, and amnestic use for perioperativeevents; conscious sedation during short diagnostic, operative orendoscopic procedures; as a component for the induction and maintenanceof general anaesthesia, prior and/or concomitant to the administrationof other anaesthetic or analgesic agents; ICU sedation.

BRIEF DESCRIPTION OF THE DRAWINGS

Preferred embodiments of the invention are described in the followingExamples with reference to the accompanying drawings in which:

FIG. 1 shows a graph of compound of formula (I) content (% relative toinitial) vs storage temperature;

FIG. 2 shows Differential Scanning calorimetry (DSC) of LJC-039-081-1;

FIG. 3 shows DSC of LJC-039-081-1 (solid) overlaid with LJC-039-081-2(dotted);

FIG. 4 shows DSC of besylate forms (Form 1 solid, Form 2 dashed);

FIG. 5 shows DSC of besylate forms (Form 1 solid, Form 3 dotted anddashed);

FIG. 6A and FIG. 6B shows chromatographs of LJC-039-037-1 at T⁰ and T⁴(and relate to the results in Table 10);

FIG. 7 shows XRPD comparing LJC-039-037-1 (besylate salt) pre and post 4week stability study;

FIG. 8A shows an XRPD comparison of besylate Form 1 and 2;

FIG. 8B shows Differential Scanning calorimetry (DSC) overlays of Form 1and 2;

FIG. 9A shows an XRPD comparison of besylate Form 1 and 3, and FIG. 9Bshows overlays of Form 1 and 3;

FIG. 10 shows DSC of LJC-039-086-1 (besylate Form 4);

FIGS. 11A-11I show results for besylate Form 1: FIG. 11A) XRPD for 100mg batch LJC-039-037-1; FIG. 11B) DSC for 100 mg batch LJC-039-037-1;FIG. 11C) TGA for 100 mg batch LJC-039-037-1; FIG. 11D) 1H NMR for 100mg batch LJC-039-037-1; FIG. 11E) GVS for 100 mg batch LJC-039-037-1;FIG. 11F) XRPD post GVS for 100 mg batch LJC-039-037-1; FIG. 11G) XRPDpost stability at 40° C./75% RH for 100 mg batch LJC-039-037-1; FIG.11H) VT XRPD for 100 mg batch LJC-039-037-1; FIG. 11I) light polarisedmicroscopy for 100 mg batch LJC-039-037-1;

FIGS. 12A-12D show results for besylate Form 2: FIG. 12A) XRPD for 100mg batch LJC-039-067-8; FIG. 12B) DSC for 100 mg batch LJC-039-067-8;FIG. 12C) DSC with ramp rate of 2° C./min; FIG. 12D)¹H NMR forLJC-039-067-8;

FIGS. 13A-13G show results for besylate Form 3: FIG. 13A) XRPD forLJC-039-081-2 (2^(nd) crop from liquors of LJC-039-081-1); FIG. 13B) DSCfor LJC-039-081-2; FIG. 13C) DSC for LJC-039-081-2 (2° C./min ramprate); FIG. 13D) TGA for LJC-039-081-2; FIG. 13E)¹H NMR forLJC-039-081-2; FIG. 13F) GVS for LJC-039-081-2; FIG. 13G) XRPD post GVSfor LJC-039-081-2;

FIGS. 14A-14C show results for besylate Form 4: FIG. 14A) XRPD forLJC-039-086-1; FIG. 14B) DSC for LJC-039-086-1; FIG. 14C)¹H NMR forLJC-039-086-1;

FIGS. 15A and 15B show HPLC chromatographs for release batch of besylatesalts, followed by FIGS. 15C and 15D showing Agilent ChemStation reportsdetailing results;

FIGS. 16A-16D show chiral chromatography for LJC-039-081-1, andLJC-039-083-1;

FIG. 17 shows exemplar images (ca. 4-8 mm diameter field of view) of thesolid forms observed in crystallisations of compound of formula (I)besylate;

FIG. 18 shows content of the asymmetric unit in Form 1;

FIG. 19 shows molecular structure as determined by single-crystal X-raydiffraction of a crystal of compound of formula (I) besylate, Form 1,grown from a 2-methoxyethanol:pentyl acetate solution with atomsrepresented by thermal ellipsoids. Only hydrogens specifically locatedin the crystal structure are depicted;

FIG. 20 shows conformation adopted by the two independent molecules inForm 1;

FIG. 21 shows comparison of the conformation adopted by one independentmolecule in Form 1 (top) and the conformation in Form 2 (bottom);

FIG. 22 shows comparison of the conformation adopted by the twoindependent besylates in Form 1, view along two different directions;

FIG. 23 shows comparison of the conformation adopted by one independentbesylate in Form 1 (top) and the conformation in Form 2 (bottom);

FIG. 24A-24C show crystal structure, determined by single-crystal X-raydiffraction of a crystal of compound of formula (I) besylate grown from2-methoxyethanol:pentyl acetate solution, viewed along thecrystallographic a axis (FIG. 24A), b axis (FIG. 24B), and c axis (FIG.24C);

FIG. 25 shows short contact C—O<3.6 Å, C—C<3.6 Å, and N—O<3.5 Å for Form1;

FIG. 26 shows calculated powder pattern diffraction from single crystalX-ray diffraction data for Form 1;

FIG. 27 shows plate form crystals observed for compound of formula (I)besylate Form 2;

FIG. 28 shows content of the asymmetric unit in Form 2;

FIG. 29 shows molecular structure as determined by single-crystal X-raydiffraction of a crystal of compound of formula (I) besylate Form 2 withatoms represented by thermal ellipsoids. Only Hydrogens specificallylocated in the crystal structure are depicted;

FIG. 30 shows conformation adopted by the independent molecule in Form2;

FIG. 31 shows conformation adopted by the independent besylate in Form2, viewed along two different directions;

FIGS. 32A-32C show a crystal structure, determined by single-crystalX-ray diffraction of a crystal of compound of formula (I) besylate Form2, viewed along the crystallographic a axis (FIG. 32A), b axis (FIG.32B), and c axis (FIG. 32C);

FIG. 33 shows short contact C—O<3.6 Å, C—C<3.6 Å and N—O<3.5 Å for Form2;

FIG. 34 shows calculated powder pattern diffraction from single crystalX-ray diffraction data for Form 2;

FIG. 35 shows labelling of atomic centres for Compound of formula (I)besylate Form 1; and

FIG. 36 shows labelling of atomic centres for Compound of formula (I)besylate Form 2.

DETAILED DESCRIPTION OF PREFERRED EMBODIMENTS Example 1

Solid-State Stability Study of Compound of Formula (I)

Method/Technique.

2 mg samples of compound of formula (I), accurately weighed, were placedin 4-mL clear glass screw-cap vials. Samples were tested at initial andafter 34 days stored at 5° C./Ambient Relative Humidity (AMRH) Closed,30° C./60% RH Closed, 40° C./75% RH Open and 60° C./AMRH Closed.

TABLE 1 HPLC Method Condition Column: Phase = Phenomenex Luna C18(2)Length × i.d = 100 × 4.6 mm Particle size = 3 μm Mobile phase: A =1000:1 Water/Trifluoroacetic Acid B = 1000:0.5Acetonitrile/Trifluoroacetic Acid Flow rate: 1.0 mL/min ColumnTemperature: 40° C. Time (min) % A % B Gradient 0.0 80 20 20.0 20 6025.0 20 60 25.1 80 20 30.0 80 20 Detection Wavelength: 230 mm SampleMass Injected μg, typically 1 μL injection of 1.0 mg compound of formula(I)/mL in 60:40 Water/Acetonitrile Retention Times Compound of formula(I) elutes at approximately 7.64 minResults

Appearance.

Table 2 lists the appearance results. Table 2. Summary of Compound ofFormula (I) Appearance Data

Timepoint Storage Condition days Appearance RT initial Cream to lightyellow powder  5 C./AMRH Closed 34 Cream to light yellow powder 30C./60% RH Closed 34 Cream to light yellow powder 40 C./75% RH Open 34Deliquesced yellow mass on bottom of vial 60 C./AMRH Closed 34Deliquesced dark yellow to orange mass on bottom of vial

Compound of Formula (I) Content (% w/w).

The % w/w content values (see Table 3) show too much variability todetect differences between the initial value and those measured after 34days at 5° C./AMRH Closed, 30° C./60% RH Closed or 40° C./75% RH Open.The average % w/w measured for the samples stored 34 days at 60° C./AMRHClosed show a 10% w/w decrease from the initial value.

Compound of Formula (I) Content (% Area).

The compound of formula (I) % area content (see Table 3 and FIG. 1)shows no significant change after 34 days stored at 5° C./AMRH Closed,but decreases steadily with increasing storage temperature for samplesat 30° C./60% RH Closed, 40° C./75% RH Open or 60° C./AMRH Closed. Majordegradation peaks are observed at RRT 0.68, 0.87 and RRT 0.90, but thechromatograms, which are relatively complex even at initial (23 peaks),also show many new small degradent peaks (e.g. 7 peaks at 30° C./60% RHClosed; 13-20 peaks at 60° C./AMRH Closed). These observations suggestmultiple degradation pathways. The degradent at RRT 0.68 is tentativelyidentified as the ester hydrolysis product (the free acid of compound offormula (I)). It is most prevalent in the 40° C./75% RH Open samples, aswould be expected for a hydrolysis product.

TABLE 3 Summary of Compound of Formula (I) HPLC Data Compound % ofFormula Relative to Timepoint (I) Content Avg. Initial Storage ConditionDays % w/w % area % area RT initial 100.5 95.14 Avg = 94.81 RT initial104.1 94.47  5 C./AMRH Closed#1¹ 34 102.6 95.30 100.52 30 C./60% RHClosed #1¹ 34 94.7 94.20 99.36 40 C./75% RH Open #1 34 105.4 93.45 98.5740 C./75% RH Open #2 34 100.3 93.39 98.50 60 C./AMRH Closed #1 34 93.487.77 92.57 60 C./AMRH Closed #2 34 91.1 87.77 92.57NotesOnly one sample was tested due to an autosampler sequencer error.Conclusions

Compound of formula (I) is stable with respect to appearance and contentfor at least 34 days stored at 5° C./AMRH Closed. No change inappearance was noted at 30° C./60% RH Closed, but an approximately 0.6%drop in compound of formula (I) content relative to the initial % areawas observed. Samples stored at 40° C./75% RH Open or 60° C./AMRH Closeddeliquesced, became yellow to orange in colour and showed notabledecreases (1.5 to 8%) in compound of formula (I) content relative toinitial. Major degradation peaks at RRT 0.68, 0.87 and RRT 0.90 areobserved along with numerous smaller peaks, suggesting multipledegradation pathways. The degradent at RRT 0.68 is tentativelyidentified as the ester hydrolysis product. These results indicate thatcompound of formula (I) should be stored refrigerated for long termstorage.

Example 2

The solubility of the compound of formula (I) was determined in a widerange of organic solvents. The solubility data is shown in Table 4below.

TABLE 4 Solvent Min solvent required/mg/ml Methanol 446 Ethanol 324Propan-2-ol 454 Acetone 214 Toluene 460 Ethyl acetate 218Tetrahydrofuran 311 Acetonitrile 362

The data clearly shows that the compound of formula (I) has highsolubility in common organic solvents. The preferred solvents areethanol and toluene.

Two basic centres of the free base of the compound were measured forpKa. However, the basic centre of the pyridine ring had a pKa of 1.99.The pKa of the basic centre of the imidazole ring was measured to be4.53.

Benzene sulfonic acid was used to produce a besylate salt of thecompound of formula (I). Experiments were conducted on a 20 mg scaleusing 6 volumes of solvent. All reactions were carried out at ambienttemperature with acids charged as stock solutions in ethanol (1M) or assolids depending on solubility.

Solids isolated showed significant peak shifts in ¹H NMR to confirm saltformation. X-Ray Powder Diffraction (XRPD) showed that the salt hadcrystalline indication. Table 5 summarises the isolated salt form.

TABLE 5 Entry Salt Solvent ID 1 besylate toluene LJC-039-009-7

The salt was subsequently stored at 40° C./75% RH for two weeks thenre-analysed by XRPD and HPLC for chemical purity to assess stability ofthe materials. The salt retained the same powder pattern after exposureto the humidity conditions, and also retained high chemical puritysupporting improved stability.

It can be seen from the T¹ purity results of the isolated salt (Table 6below) that the besylate salt from toluene showed high purity valuesbefore and after the stability study.

TABLE 6 Summary of purity before and after 40° C./75% RH for 1 weekEntry Salt ID Purity T⁰/% Purity T¹/% 1 besylate LJC-039-009-7 95.9 95.9

The results above show that the besylate salt form showed high purityand favourable stability results.

Example 3

Scale up of the besylate salt to 100 mg was performed based on data inExample 2. Toluene was found to be the preferred solvent for isolatingbesylate salts.

Besylate Salt of Compound of Formula (I)

A scale up to 50 mg of input material was carried out in order toconfirm whether or not the process would scale up, and to confirm thatthe material isolated was of the same crystalline form (Form 1) seenfrom the previous smaller scale experiment. Once the analysis confirmedthe salt to be Form 1 and that the properties were in keeping with whatwas expected, another scale up was carried out with 100 mg of inputmaterial in order to carry out full characterisation and submit thesample for a 4 week stability study at 40° C./75% RH. Both the scaled upreactions were carried out in toluene with benzene sulfonic acid addedas a solution in ethanol (1M).

Besylate Experimental Procedure

Compound of formula (I) free base (100 mg, batch 704-17) was charged toa vial and toluene (600 μl) was added at ambient temperature. To thesolution benzene sulfonic acid (250 μl, 1M in ethanol) was added and thereaction mixture stirred for fifteen minutes, after which time a solidhad precipitated from the solution which was filtered, washed withtoluene and oven dried at 40° C. under vacuum. Analysis by XRPD showedthe solid to be of identical powder pattern as other besylatesgenerated, and the ¹H NMR confirmed salt formation due to significantpeak shifts.

TABLE 7 Onset TGA Chiral GVS melt/ weight Solubility Chemical purity/%Entry ID salt uptake/% ° C. loss/% mg/ml purity/% e.e 1 LJC- besylate2.0 201.3 4.9 8.3 97.1 94.4 039- 037-1

The enantiomeric excess for LJC-039-037-1 was only 94.4 therefore theresult was compared to another batch of besylate (LJC-039-081-1) thatwas isolated under identical conditions. The enantiomeric excess of thisbatch was 99.1%.

Process Optimisation

To improve further yields of besylate salt (Form 1) four solvents werescreened (isopropyl acetate, ethyl formate, methanol and acetone). Intotal eight 100 mg scale reactions were conducted in these solvents withthe relevant acid added as stock solution in ethanol for comparison toprevious experiments.

Compound of formula (I) (batch 704-38, 100 mg) dissolved in solvent (600μl) at ambient. Acid (250 μl, 1M stock solution in ethanol) added andall reaction mixtures stood for 48 hours at ambient. The results aresummarised in Table 8.

TABLE 8 Results of process optimisation experiments Purity post 40°C./75% Table Lab book Purity/ RH for 4 entry reference Salt Solvent XRPDYield/% % area weeks 1 LJC-039- besylate acetone Form 1 38 98.4 98.1067-2 2 LJC-039- besylate iPrOAc Form 1 79 97.7 95.9 067-4 3 LJC-039-besylate Ethyl Form 1 40 98.6 98.3 067-6 formate 4 LJC-039- besylateMeOH Single Not 98.1 Not 067-8 crystals, recorded recorded Form 2

All reactions except that of besylate formation in methanol showedForm 1. The methanol reaction was stored at 4° C. The data obtainedconfirmed anhydrous besylate 1:1, and a powder pattern of the materialconfirmed the existence of a new form (Form 2).

It was concluded from the study that solvents such as isopropyl acetateincreased the purity of the salts, however reduced the recovery. Becausethe previous choice of solvent (ethyl acetate) gave high yielding saltswith high purity values, it was decided to use ethyl acetate for thefinal scale up experiments.

Besylate (Form 1) 1 g Scale-Up

A 1 g formation of the besylate salt was carried out. This successfullyproduced 950 mg (70% yield) of Form 1. The liquors were highly coloured(yellow) and therefore seeded with a small amount of Form 1, to assistrecovery. The liquors were stored at 4° C. for 16 hours. The solidobtained displayed a new powder pattern (Form 3). The solid was analysedby thermal analysis and variable temperature XRPD to confirm whether ornot it was a true polymorph or a solvate. Interpretation of the analysisconcluded it not to be a solvate from the ¹H NMR evidence, and the DSCshowed two endothermic events confirmed by hotstage microscopy (FIG. 3).It was interpreted that the seeds of Form 1 melted at 187° C., with Form3 melting at 200° C. The reason that Form 1 was not identified by XRPDis that this is a less sensitive technique than microscopy.

Form 3 precipitates at a lower temperature to Form 1.

Characterisation was carried out on the polymorphs to propose therelationship between them.

TABLE 9 Thermal data of besylate forms Entry ID Form Onset of Melt/° C.ΔH/Jg⁻¹ 1 LJC-039-081-1 1 201 56 2 LJC-039-067-8 2 180 73 3LJC-039-081-2 1, 3 187, 200 7.6, 37The lower melting point of the small amount of Form 1 present inLJC-039-081-2 can be potentially attributed to lower purity (97.2%compared with 97.9% in LJC-039-081-1).

FIG. 4 shows the DSC of besylate forms 1 (solid) and 2 (dashed).

FIG. 5 shows the DSC of besylate forms 1 (solid) and 3 (dotted anddashed).

Example 4

Salt Stability Studies

TABLE 10 Summary Table of salt purities after 4 week stability studySample ID salt T⁰ T¹ T² T³ T⁴ LJC-039-037-1 besylate 97.1 97.3 97.4 96.796.7

Crystalline samples of besylate were stored at 40° C./75% RH for a totalof four weeks and samples were taken for HPLC every seven days. Thebesylate hplc purity remained consistent up until T³ when it reached96.7%. This value did however remain consistent to T⁴.

The hplc chromatographs for the besylate salt form are shown in FIG. 6for time points week zero and week four.

It is suspected that the dominant peak prior to that of the parent isfrom contamination as the λ_(max) does not match the λ_(max) of theparent peak. It is also absent from the impurity profile of T¹, T², T³and T⁴.

It can be seen from the powder patterns of the salts pre and posthumidity studies that there are no changes in form.

FIG. 7 shows XRPD comparing LJC-039-037-1 (besylate salt) pre and post 4week stability study.

Example 5

Polymorphism Investigation

In order to determine the propensity of besylate salts to exhibitpolymorphism, a maturation experiment was set up using thirty solvents(fifteen neat plus their 2.5% aqueous counterparts). The solid wasslurried in various solvents (see Table 11) for one week on a heat/coolcycle from ambient to 60° C. After one week the slurries were evaporatedand the solids analysed by XRPD and HPLC.

TABLE 11 Results of polymorphism investigation for besylate(LJC-039-058-2) starting hplc purity 97.7% Entry solvent XRPD post 1week HPLC purity/% area 1 acetone Form 1 97.5 2 THF Form 1 97.6 3 IPAamorphous 97.1 4 MtBE Form 1 97.7 5 DCM amorphous 97.4 6 EtOH oil notanalysed 7 MEK Form 1 97.2 8 1,4-Dioxane Form 1 97.2 9 iPrOAc Form 197.5 10 DMF oil not analysed 11 MeCN Form 1 94.3 12 nBuOH oil notanalysed 13 nPrOH oil not analysed 14 MIBK Form 1 97.7 15 MeOH oil notanalysed 16 2.5% aq acetone Form 1 96.8 17 2.5% aq THF amorphous 93.3 182.5% aq IPA Form 1 76.1 19 2.5% aq MtBE oil not analysed 20 2.5% aq DCMForm 1 97.4 21 2.5% aq EtOH oil not analysed 22 2.5% aq MEK Form 1 93.923 2.5% aq 1,4-Dioxane Form 1 86   24 2.5% aq iPrOAc oil not analysed 252.5% aq DMF oil not analysed 26 2.5% aq MeCN Form 1 93.3 27 2.5% aqnBuOH oil not analysed 28 2.5% aq nPrOH oil not analysed 29 2.5% aq MIBKForm 1 97.3 30 2.5% aq MeOH oil not analysed

The maturation study using the besylate salt revealed no new forms. Thepurity results post maturation show that those slurried in acetonitrile,aqueous THF, aqueous IPA aqueous MEK, aqueous dioxane and aqueousacetonitrile degraded. This suggests that the besylate salt (Form 1) hasgood solution stability in neat organic solvents at high temperature.

Investigating New Forms of Besylate

Although no new forms of the besylate salt were seen from the maturationstudy, a new form was seen when crystals were grown in methanol. Thesingle crystals obtained from methanol were ground in order to obtain apowder pattern. This pattern turned out to be different from Form 1. Arepeat experiment was carried out in order to obtain a further supply ofForm 2. It was only possible to isolate Form 2 from precipitation over16 hours from the liquors, opposed to allowing the solvent to evaporate,this gave Form 1. Interestingly two habits were present; needles andblocks. Both showed the same powder pattern as the needle habit that wasused for single crystal structure determination.

Full analysis was carried out on Form 2. It had been concluded that itwas a true polymorph as the single crystal data confirmed anhydrousbesylate 1:1.

FIG. 8A shows an XRPD comparison of besylate Form 1 and 2. There is anobvious difference between Form 1 (trace 1) and Form 2 (trace 2). As canbe seen from the two powder patterns, both forms are very different.Thermal analysis was carried out to compare the melting points of thetwo forms and also thermodynamic solubility measurements recorded.

FIG. 8B shows overlays of Form 1 and 2. Form 1 and 2 show oneendothermic event (melting).

Form 3 was identified when a second crop was isolated from the liquorsof LJC-039-081-1 (the 1 g scale-up reaction). Analysis was carried outin order to determine whether or not it was a solvate and how the formsinterconvert.

FIG. 9A shows an XRPD comparison of besylate Form 1 and 3. FIG. 9B showsoverlays of Form 1, and 3.

Form 1 shows one endothermic event (melting), whereas Form 3 shows twoevents. Hotstage microscopy on Form 3 clearly shows two melts within 20°C. of each other. It is postulated that a small amount of the lowermelting polymorph is present as it was not picked up in variabletemperature XRPD, which is a less sensitive technique. It is quitepossible that the first endothermic event represents Form 1 as it wasused to seed the liquors that Form 3 was isolated from.

The solubility data shows that all three forms have very similar aqueoussolubilities of 7.8 to 8.3 mg/ml at pH 3.

Besylate Salt Form 4

The release batch of besylate salt Form 1 (LJC-039-083-1) was of highpurity (97.6%), but contained a small amount of impurity carried throughfrom the free base (0.78%, 11.9 min RT). This impurity was observed inthe DSC experiment showing an endothermic transition (onset at 130° C.).The peak was confirmed as having an unrelated λmax to that of the parentpeak.

A 100 mg sample was taken for a re-crystallisation attempt from 40%isopropyl acetate/ethanol. The re-crystallisation was carried outtraditionally by dissolving the salt in the minimum amount of hotsolvent, then cooling slowly to ambient to yield a precipitate. Thedried solid was analysed by XRPD which indicated a new form, and withthermal analysis and ¹H NMR it was confirmed to be a polymorph and not asolvate. FIG. 10 shows DSC of LJC-039-086-1.

The salt screen investigations have shown that compound of formula (I)forms many salts within the appropriate pKa range, and that they areeasily isolated from a range of solvents. From full characterisation ofthe salts, it has been determined that the besylate salts have goodstability with respect to humidity. It has been concluded that there aretwo polymorphic forms of besylate. Form 3 came from the second crop ofLJC-039-081-1 liquors after seeding with Form 1. Form 4 has beenobserved after a re-crystallisation of Form 1 was carried out from 40%isopropyl acetate/ethanol.

Full analytical data is shown in FIGS. 11-14 below.

Experimental Methods for Examples 2-5 Example 2

Compound of formula (I) (5 mg/well) was dissolved in solvent (ethanol,toluene, and acetonitrile) (30 μl) in HPLC vials. To the solutions,benzene sulfonic acid (11.4 μl, 1M in ethanol) was added and thereaction mixtures stood overnight at ambient. Those vials that containedsolid were dried at 40° C. under vacuum, and those that remained assolutions were concentrated by evaporation and then treated withheptane. Those that precipitated were dried as mentioned, and those thatoiled were stored at 4° C.

Besylate Form 1 Scale Up

Compound of formula (I) (100 mg) dissolved in ethyl acetate (600 μl) andbenzene sulfonic acid (250 μl, 1M in ethanol) added. Precipitationoccurred instantly and the reaction mixture was stirred for 24 hours atambient. The solid was filtered, washed with ethyl acetate and ovendried at 40° C. under vacuum for 16 hours.

Analysis Methods

Differential Scanning Calorimetry (DSC)

DSC data was collected on a TA instrument Q1000 equipped with a 50position autosampler. The energy and temperature calibration standardwas indium. Samples were heated at a rate of 10° C./min between 25 and350° C. A nitrogen purge at 30 ml/min was maintained over the sample.

Between 0.5 and 3 mg of sample was used, unless otherwise stated, andall samples ran in a pin holed aluminium pan.

Thermogravimetric Analysis (TGA)

TGA data was collected on a TA Instrument Q500 TGA, calibrated withAlumel and running at scan rates of 10° C./minute. A nitrogen purge at60 ml/min was maintained over the sample.

Typically 5-10 mg of sample was loaded onto a pre-tared platinumcrucible unless otherwise stated.

NMR

All spectra were collected on a Bruker 400 MHz equipped withautosampler. Samples were prepared in d6-DMSO, unless otherwise stated.

XRPD (X-Ray Powder Diffraction)

Bruker AXS C2 GADDS Diffractometer

X-ray powder diffraction patterns for the samples were acquired on aBruker AXS C2 GADDS diffractometer using Cu Kα radiation (40 kV, 40 mA),automated XYZ stage, laser video microscope for auto-sample positioningand a HiStar 2-dimensional area detector. X-ray optics consists of asingle Göbel multilayer mirror coupled with a pinhole collimator of 0.3mm.

Beam divergence, i.e. the effective size of the X-ray beam on thesample, was approximately 4 mm. A θ-θcontinuous scan mode was employedwith a sample to detector distance of 20 cm which gives an effective 2θrange of 3.2-29.8°. A typical exposure time of a sample would be 120 s.

Samples run under ambient conditions were prepared as flat platespecimens using powder as received without grinding. Approximately 1-2mg of the sample was lightly pressed on a glass slide to obtain a flatsurface. Samples run under non-ambient conditions were mounted on asilicon wafer with heat conducting compound. The sample was then heatedto the appropriate temperature at ca. 20° C./minute and subsequentlyheld isothermally for ca 1 minute before data collection was initiated.

Purity Analysis:

Chemical Method

Purity analysis was performed on a HP1100 Agilent:

Method: Gradient, Reverse Phase

Method Duration/min: 34

Column: Phenomenex Gemini C18 5 μm (2.0×50 mm) (Guard cartridgePhenomenex

Gemini C18 guard cartridge 2×4 mm)

Column Temperature/° C.: 40

Injection/μl: 5

Flow Rate ml/min: 0.8

Detection: UV

Wavelength/nm: 255 (bandwidth of 90 nm), 240 (bandwidth of 80 nm), 254(bandwidth of 8 nm)

Phase A: 2 mmol NH₄HCO₃ (adjusted to pH10 with NH₃ solution)

Phase B: acetonitrile

Timetable:

Time/Min % A % B 0 90 10 25 10 90 28.8 10 90 29 90 10 34 90 10

Chiral Method

Purity analysis was performed on a Gilson HPLC system:

Method: Isocratic, Normal Phase

Method Duration/min: 50

Column: Diacel Chiralcel OJ-H (5 μm) 4.6×250 mm (Guard cartridge DiacelChiralcel

OJ-H analytical guard cartridge 5 μm 4.0×10 mm)

Column Temperature/° C.: 40

Injection/μl: 10

Flow Rate ml/min: 1.0

Detection: UV

Wavelength/nm: 225 (single wavelength detector)

Phase A: hexane

Phase B: ethanol

Timetable:

Time/Min % A % B 0 93 7Gravimetric Vapour Sorption (GVS) Studies

All samples were run on a Hiden IGASorp moisture sorption analyserrunning CFRSorp software. Sample sizes were typically 10 mg. A moistureadsorption desorption isotherm was performed as outlined below (2 scansgiving 1 complete cycle). All samples were loaded/unloaded at typicalroom humidity and temperature (40% RH, 25° C.). All samples wereanalysed by XRPD post GVS analysis. The standard isotherm was performedat 25° C. at 10% RH intervals over a 0-90% RH range unless otherwisestated.

Scan1 Scan2 Adsorption Desorption Adsorption 40 85 10 50 75 20 60 65 3070 45 40 80 35 90 25 15 5 0Solubility

This was measured by suspending sufficient compound in 0.25 ml ofsolvent (water) to give a maximum final concentration of 10 mg/ml of theparent free form of the compound. The suspension was equilibrated at 25°C. for 24 hrs followed by a pH check and filtration through a glassfibre C 96 well plate. The filtrate is then diluted down 101×.Quantitation was by HPLC with reference to a standard dissolved in DMSOat approx 0.1 mg/ml. Different volumes of the standard, diluted andundiluted tests were injected. The solubility was calculated byintegration of the peak area found at the same retention time as thepeak maximum in the standard injection. If there is sufficient solid inthe filter plate the XRPD is normally checked for phase changes, hydrateformation, amorphization, crystallization etc.

Timetable:

Time/min % Phase A % Phase B 0.0 95 5 1.0 80 20 2.3 5 95 3.3 5 95 3.5 955 4.4 95 5pKa Determination

pKa determination was performed on a Sirius GlpKa instrument with D-PASattachment. Measurements were made by potentiometric titration inMeOH:H2O mixtures at 25° C. The titration media was ionic strengthadjusted with 0.15M KCl. The values found in the MeOH:H₂O mixtures wereextrapolated to 0% co-solvent via a Yasuda-Shedlovsky extrapolation.

Hot Stage Microscopy

Hot stage microscopy was studied using a Leica LM/DM polarisedmicroscope combined with a Mettler-Toledo MTFP82HT hot-stage in thetemperature range 25-350° C. with typical heating rates in the range10-20° C./min. A small amount of sample was dispersed onto a glass slidewith individual particles separated as well as possible. Samples wereviewed under normal or cross-polarised light (coupled to a λfalse-colour filter) with a ×20 objective lens.

Chiral Purity Method

System Setup

Pump: Gilson 322 binary pump

Detector: Gilson 152 UV/Vis

Autosampler: Gilson 233XL rack+Gilson 402 dual syringe pump

Column oven: Phenomenex Thermasphere TS-130

Software: Gilson Unipoint LC software

Column: Daicel Chiralcel OJ-H, 5 μm, 4.6×250 mm

Guard column: Daicel Chiralcel OJ-H analytical guard cartridge, 5 μm,4.6×10 mm

HPLC Conditions

Channel A: Hexane (93%)

Channel B: Ethanol (7%)

Flow rate: 1.0 ml/min

Detector wavelength 225 nm

Column Temperature: 40° C.

Run time: 50.0 mins

Sample Conditions

Approximately 0.2 mg of sample was dissolved in the appropriate volumeof Hexane:Ethanol 1:1 v/v to give a 0.2 mg/ml solution. This was cappedand placed on a vortex mixer at high speed for a duration of ˜15seconds. If solid remained at this point, then the sample vial wassonicated for approximately 10 seconds followed by a further 10 to 15seconds on the vortex mixer. 10 μl was injected onto the HPLC system.Samples were injected in duplicate following an initial duplicateinjection of Hexane:Ethanol 1:1 v/v as a blank.

Example 5

Pharmacological Test Example

The anaesthetic and sedative effects of the besylate salt Form 1 of thepresent invention was evaluated. The besylate (benzenesulfonic acid)salt was dissolved in physiological saline for administration of thetest composition to the animal. The test composition was administered tomice, placed in individual Plexiglas cages (20×10×10 cm). Mice wereinjected with either vehicle or test substance by the intravenous route.The latency to sleep and the duration of anaesthesia (maximum: 90minutes after test-substance administration) were recorded. Anaesthesiais indicated by loss of the righting reflex (LRR). The righting reflextest was performed as soon as the animals appear sedated, approximatelyevery 20-30 seconds. Once the righting reflex is absent, duration ofloss of righting reflex was measured by testing for the return of therighting reflex approximately every 20-30 seconds thereafter. Eight micewere studied per group and the test was performed blind. Results fromthe study are given in the table below.

LATENCY TO NUMBER LRR TREATMENT OF MICE (min) LRR DURATION(##) (mg/kg)WITH mean ± (min) i.v. LRR s.e.m. (#) mean ± s.e.m. (#) p value Vehicle0 — 0.0 ± 0.0 — CNS 7056X 2 — 1.7 ± 1.3 NS 0.1441 besylate (20.4) CNS7056X 5+ 3.0 ± 0.2 4.9 ± 1.6* 0.0106 besylate (27.2) CNS 7056X 6++ 1.8 ±0.2 6.0 ± 1.9** 0.0038 besylate (34) CNS 7056X 6++ 1.6 ± 0.5 7.3 ± 2.5**0.0038 besylate (40.8) Mann-Whitney U test: NS = Not Significant; *= p <0.05; **= p < 0.01 Fisher's Exact test (number of mice with LRR): noindication = not significant; += p < 0.05; ++= p < 0.01 (#): notcalculated if n < 3 (##): maximum = 90 minutes after injection

The results in the above table show that the besylate salt Form 1 has ashort latency to loss of righting reflex and therefore a short inductiontime to anaesthesia in the animals. Additionally the mice recoverrapidly from anaesthesia as indicated by the short duration of loss ofrighting reflex. Thus, this compound can provide rapid induction andrecovery from anaesthesia.

Example 6

Additional Conditions for Crystallisation of Forms 2, 3, and 4

Additional conditions were tested in an attempt to reproduce thepreviously reported crystallisations of Forms 2, 3 and 4. However, thereported scales were substantially reduced and the methodology modifiedaccordingly, as described below.

Form 2

5 mg of solid was dissolved in 25 ul of methanol and 10 ul of ethanoladded; the solution was then chilled at 4° C. for 3 days.

Form 3

Three variants were attempted:

5 mg of solid was dissolved in 50 ul of ethanol and 120 ul of ethylacetate added; the solution was then chilled at 4° C. for 3 days.

10.1 mg of solid was dissolved in 300 ul of ethanol and 120 ul of ethylacetate added; the solution was then chilled at 4° C. for 3 days.

2.5 mg of solid was dissolved in 50 ul of ethanol in a silanized vialand 100 ul of ethyl acetate added; the solution was then chilled at 4°C. for 3 days.

Form 4

Three variants were attempted:

A warmed (70° C.) mixture isopropyl acetate:ethanol (40%:60% v/v) wasadded to 5 mg of warmed solid in 20 ul aliquots until the soliddissolved (60 ul of solvent mixture in total); the solution was thenallowed to cool slowly to ambient in a thermostated waterbath initiallyat 70° C. over a period of hours.

5 mg of solid was dissolved in 180 ul of warmed (50° C.) isopropylacetate:ethanol (40%:60% v/v) solvent and the solution allowed to coolslowly to ambient in a thermostated waterbath (initially at 50° C.) overa period of hours.

5 mg portion of solid was dissolved in 100 ul of warmed (50° C.)isopropyl acetate:ethanol (40%:60% v/v) solvent in a silanized vial andthe solution allowed to cool slowly to ambient in a thermostatedwaterbath (initially at 50° C.) over a period of hours.

Each of the crystallisations yielded solid material with blade andplate-like habits, with the Form 4 crystallisations also yieldingneedle-like material.

Example 7

Characterisation of Compound of Formula (I) Besylate

Compound of formula (I) besylate is chiral and assumed to be of thesingle enantiomeric form below, i.e. the S enantiomer (consistent withthe subsequently determined crystal structures):

The heterocyclic structure contains a basic Nitrogen in the imidazolering (pKa of ca. 5), and a weaker basic Nitrogen in the pyridyl ring(pKa of ca. 2). The imidazole-Nitrogen will typically be protonated inthe presence of the strongly acidic besylate (pKa ca. −0.6) in aqueoussolution, with the pyridyl-Nitrogen also potentially being protonatedunder conditions of excess besylate.

The neutral free base form (i.e. unprotonated) of the compound isexpected to be somewhat lipophilic (log P_(octanol:water) ca. 4.0) andthus would prefer some lipophilic environments over aqueous ones.Moreover, it is likely to retain a degree of lipophillicity even whenmonoprotonated (log D_(octanol:water) ca. 2 at pH3), although the effectof the besylate counter-ion is likely to ameliorate this tendencythrough its inherent hydrophilicity. The degree of lipophilicity furtherdiminishes for the diprotonated form (log D_(octanol:water) ca. 0.6 atpH0).

The compound also has an excess of Hydrogen bond acceptors and thereforewill be suitably partnered by Hydrogen bond donating solvents. It isthus expected that the compound will prefer solubilisation in a range ofpolar organic solvents such as the alcohols, particularly those whichprovide a partially lipophilic, Hydrogen bond donating environment. Thishas been borne out by experimental evidence (details of solvents usedare given in Example 8):

Observed solubility Solvent (mg/ml) Formamide 350 Water 2 Dimethylsulfoxide 500 Dimethylacetamide 200 1,2-ethanediol 60 Dimethylformamide300 Acetonitrile >20 Methanol 400 2-ethoxyethanol 202,2,2-trifluoroethanol 1000 Ethanol 100 Acetone 2 Propan-1-ol 15Propan-2-ol 4.8 2-methoxyethanol 167 Hexafluoropropan-2-ol >700Dichloromethane <<0.3 Tetrahydrofuran 2.5 Methylbenzoate 2 Ethyl acetate0.2 Chloroform <<0.4 1,4-dioxan 1 Soluble (>5 mg/ml), partially soluble(2.5-5 mg/ml), partially insoluble (0.5-2.5 mg/ml, insoluble (<0.5mg/ml). Values quoted are approximate, but experimentally confirmed.

These results highlight the good solubility of the compound in a widevariety of polar organic solvents. In particular, 2,2,2-trifluoroethanoland hexafluoropropan-2-ol are both identified as extremely good solventsfor this compound. This is consistent with the considerations discussedabove, both solvents being strong Hydrogen bond donors. Likewise, themore substantially lipophilic solvents are identified as poor solventsand thence potential anti-solvents for crystallisations.

Example 8

Compound of Formula (I) Besylate Crystallisations

Various conditions conducive to obtaining crystalline material ofcompound of formula (I) besylate Forms 1 and 2 are described.Crystallisation conditions which include alcohols or acetonitrilesolvents as components, with their respectively compatible anti-solventsor co-solvents, are believed to provide the most promising conditions toyield useful crystalline material. Crystallisation usingsolvent/anti-solvent binary mixtures was primarily used.Crystallisations were performed by retarded evaporation fromsub-saturated solutions of the compound in solvent/anti-solventmixtures, at ambient and reduced (4° C.) temperature. Crystallisationwas typically observed within 3-5 days of preparation.

Where sample quantity allowed, all crystallisation conditions wereperformed in duplicate in a glass 96-wellplate format; one half of eachwellplate being used to duplicate the conditions in the other half ofthe wellplate. Cross-contamination between wells is minimised by design.All of the conditions tested behaved reproducibly in at least duplicate,most yielding solid material suitable for further analysis.

In all cases, equipment coming into contact with samples andcrystallisation media were scrupulously cleaned with a variety ofsolvents and reagents before being bathed in ethanol and blown dry usingcopious evaporated nitrogen.

High quality solvents from commercial suppliers were employed, asdescribed in Table 12.

TABLE 12 Cat. Solvent Supplier No. Batch No. Grade Purity1,2-dichlorobenzene Romil H177 E558470 SpS >99.8% 1,4- Fluka 95682429739/1 puriss p.a.   >99% dimethylbenzene 1,4-dioxan Romil H297H540480 SpS >99.9% 2,2,2- Romil H860 M538412 SpS >99.9% trifluoroethanolacetonitrile Romil H049 D531490 SpS >99.9% dimethylacetamide Romil H249B540480 SpS >99.9% dimethylsulfoxide Romil H280 W530480 SpS >99.9%ethanol Romil H314 O533480 SpS >99.8% ethyl acetate Romil H346 T533480SpS >99.9% methyl iso-butyl Romil H446 M539430 SpS >99.9% ketonen-nonane Romil H568 O558450 SpS >99.9% pentylacetate Fluka 46022 13248/1puriss p.a. >98.5% propan-1-ol Romil H624 G531460 SpS >99.9% propan-2-olRomil H625 O530480 SpS >99.9% tetrachloroethylene Romil H702 W536450SpS >99.9% tetrahydrofuran Romil H718 B532470 SpS >99.9% Acetone RomilH031 E559470 SpS >99.9% Chloroform Romil H135 B554470 SpS >99.9%Dichloromethane Romil H202 O554460 SpS >99.9% Dimethylformamide RomilH253 T546460 SpS >99.9% Formamide Romil H351 Q537480 BioPure >99.9%Hexafluoropropan- Romil H359 H559470 SpS >99.9% 2-ol MethylbenzoateFluka 12460 417868/1 purum   >98% water Romil H950 D537480 SpS >99.9%

Visual analysis of the resulting crystalline morphologies was achievedusing a binocular microscope (ca. 10×-40× magnification) with digitalcamera attached, employing both transmitted and reflected lighting asappropriate.

Visual characterisation of the solid material is summarised in Table 14below. A predominance of blade or tabular/plate morphologies, either asunique crystals or as spherulites, was observed. Over all, there waslittle morphological difference between the crystallisations performedat ambient temperatures and those at 4° C., with the exception of thosewith ethanol as solvent where the tendency for spherulite and interfacetype growth diminished with lowered temperature. It is notable that theuse of anti-solvent can improve the quality of the crystalline materialsubstantially.

Example images of the crystalline material observed are presented inFIG. 17. As illustrated in this Figure, acetonitrile has a tendency toproduce spherulite growth, typically seen as a consequence of poornucleation and thence growth from poor quality crystal surfaces. Incontrast, 2-methoxyethanol has a tendency to produce unique crystals ofblade/needle-like morphology.

There appears to be a general preference for Form 1 to crystallise frommany of the conditions. However, it is notable that Form 2 has also beenobserved from several crystallisation conditions, including thescaled-down analogues for obtaining Forms 3 and 4 (described in Example6). Form 2 is observed in conditions where there are extremes of eitherpolarity (acetonitrile:water) or lipophilicity (n-nonane) or both(dimethyl sulfoxide:1,2-dichlorobenzene). In general, the crystals ofForm 2 were notable in their superior quality and distinctivewell-formed plate/tabular habit.

Single Crystal X-Ray Diffraction Cell Determinations

To provide corroborative evidence of the crystalline forms generated,the cell parameters of a number of crystals of suitable quality weredetermined using single crystal X-ray diffraction. Crystal unit cellparameters were determined using a Kappa CCD diffractometer with Moradiation, the crystals mounted on a glass fibre with oil and held at260K. The parameters for Form 1 and Form 2 have been determined assummarised in Table 13.

TABLE 13 Cell parameters determined for crystals of compound of formula(I) besylate. Form 1 Form 2 Crystal State Solvent 2-methoxyethanolethanol Anti-solvent/Co- pentyl acetate ethyl acetate solvent CrystalMorphology needle plate Crystal Size (mm) 0.8 × 0.04 × 0.02 0.7 × 0.3 ×0.25 Colour colourless colourless Crystal Structure System monoclinicorthorhombic Unit Cell a (Å)  7.6868(1)  8.92130(10) b (Å) 29.2607(5)11.1536(2) c (Å) 12.3756(3) 25.8345(4) α (°) 90 90 β (°) 97.7880(8) 90 γ(°) 90 90 Volume (Å³) 2757.86(9) 2570.65(7)

The crystallisation results from solvent/co-solvent andsolvent/anti-solvent conditions for compound of formula (I) besylatewith single crystal X-ray diffraction unit cell results are tabulated inTable 14.

TABLE 14 Experimental crystallisation results from solvent/co-solventand solvent/anti-solvent conditions for compound of formula (I)besylate, with single crystal X-ray diffraction unit cell results (X-rayresults for ambient crystallisations unless otherwise stated). ObservedX-ray Co/Anti-solvent Crystallisations Form (No & habit Solvent (&conditions) Habit of crystals) methanol ethanol (at 4° C., 3 blades &plates 2 (hex, blade) days) ethanol ethyl acetate (at blades & plates 2(4 plates) 4° C., 3 days) ethanol ethyl acetate blades & plates 2 (6plates) isopropyl acetate ethanol (70° C. → blades, plates & 2 (2plates) 20° C.) needles isopropyl acetate ethanol (50° C. → blades &plates 2 (2 hex 20° C.) plates, 2 plates, 2 blades) ethanol methylisobutyl tabular plates 2 (3 plates) ketone (at 4° C., 3 days, silanizedvial) ethanol p-cymene (at 4° C., 3 plate & tabular 2 (2 tabular) days,silanized vial) nonane none (silanized vial) blades & plates 2 (plate)dimethylsulfoxide 1,2- intergrown blades 2 (tabular) dichlorobenzenedendrite, one huge tabular dimethylacetamide methyl isobutyl plate-like1 (blade) ketone fragments dimethylacetamide tetrachloroethyleneintergrown blades 1 (2 blades) acetonitrile water interface 2 (2tabular) acetonitrile 3-methylbutan-1-ol triangular plates, 1 (blade)fragments & dendrite acetonitrile 1,2- spherulite blades 1 (2 blades)dichlorobenzene acetonitrile pentyl acetate spherulite blades 1 (blade)methanol none interface plates 2 (plate) methanol 3-methylbutan-1-oltriangular plates & 1 (2 blades) fragments methanol methyl isobutylfragments & blade 1 (blade) ketone 2,2,2- 1,2- interface & blade 1(trans, trifluoroethanol dichlorobenzene opaque & blade) translucentblades 2,2,2- 1,4- plate-like 1 (sph, plate) trifluoroethanoldimethylbenzene fragments ethanol methyl isobutyl interface plates 1(interface), ketone (5° C.: tabular & 2 (tabular) plate) ethanol 1,2-interface plates, 2 (plate) dichlorobenzene (5° C.: needles) ethanoltetrachloroethylene interface (5° C.: 2 (blade 4° C.) hexagonal tabular)ethanol 1,4- interface blades 1 (blade) dimethylbenzene propan-1-ol noneplate-like 1 (plate) fragments propan-1-ol 1,2- interface 1 (blade)dichlorobenzene propan-1-ol tetrachloroethylene plate-like 1 (blade)fragments & interface propan-2-ol 1,2- fan needles & 1 (blade)dichlorobenzene dendrite propan-2-ol n-nonane blades, needles & 1(needle) spherulite needles 2-methoxy water blade 1 (2 blades) ethanol2-methoxy pentyl acetate needles 1 (blade) ethanol 2-methoxy 1,4- blades& needles 1 (blade) ethanol dimethylbenzene 2-methoxy n-nonane blades &dendrite 1 (blade) ethanol tetrahydrofuran water plate 1 (plate)tetrahydrofuran 3-methylbutan-1-ol intergrown blades 1 (plate)tetrahydrofuran 1,2- prismatic tabular, 2 (3 tabular) dichlorobenzenefragments, powder tetrahydrofuran ethyl acetate dendrite, interface 2(plate 4° C.) tetrahydrofuran isopropyl acetate intergrown plates 1(plate) & intergrown blades tetrahydrofuran 1,3- intergrown blades 1(blade) dimethylbenzene 1,4-dioxane pentyl acetate triangular plates, 1(2 tri plate) some part of spherulite 1,4-dioxane 1,4- blade 1 (blade)dimethylbenzene

A variety of crystals of suitable quality for full single crystal X-raydiffraction crystal structure determination were achieved and the fullstructure obtained for Forms 1 and 2. These crystal structures arereported in Examples 9 and 10.

Example 9

Crystal Structure of Form 1

Crystals of compound of formula (I) besylate grown from a2-methoxyethanol:pentyl acetate solution which have a needle habit, areimaged in FIG. 17.

A single needle habit crystal (ca. 0.8×0.04×0.02 mm in size) wasselected and its cell parameters determined at 260K and then at 190K. Notransition was observed on lowering the temperature between 260-190K.The structure analysed here is for the data at 190K; parameters of thecrystal and the X-ray diffraction refinement are given in Table 15.

TABLE 15 Data of the 2-methoxyethanol:pentyl acetate grown crystal ofcompound of formula (I) besylate, Form 1. Crystal State Code CNS7056besylate Solvent 2-methoxyethanol Anti-solvent/Co-solvent pentyl acetateCrystal Morphology needle Crystal Size (mm) 0.8 × 0.04 × 0.02 Colourcolourless Crystal Structure Formula C₅₄H₅₀Br₂N₈O₁₀S₂ Formula Weight1194.98 System monoclinic Space Group P 2₁ Unit Cell a (Å)  7.6868(1) b(Å) 29.2607(5) c (Å) 12.3756(3) α (°) 90 β (°) 97.7880(8) γ (°) 90Volume (Å³) 2757.86(9) Z (No. molecules in unit) 2 Z′ (No. molecules inasymmetric 2 unit) Density (g cm³) 1.439 Absorption μ [MoKα] (mm⁻¹)1.610 F(000) 1224 Data Collection Temperature, (K) 190 Instrument KappaCCD diffractometer Scan Type ω Absorption Correction Type multi-scan No.of Measured Reflections 9868 No. of Independent Reflections 9848 θmin/max (°)  1.80/27.49 h min/max −9/9 k min/max −37/36 l min/max −15/15Refinement Refinement On F I/σ(I) Cut-off 3 No. of Used Reflections 6821No. of Parameters 686 R factor (%) 6.34 Rw factor (%) 6.39 S 1.00Δρ(min) Å⁻³ −0.8 Δρ(max) Å⁻³ 0.8 Max Shift/Error 0.0005 Flack Parameter  0.027(11)

The content of the asymmetric unit is displayed in FIG. 18. It consistsof two independent molecules of the compound and two independentbesylate counter ions. Each compound has the imidazole-Nitrogenprotonated.

The Flack “Enantiopole” parameter was determined as 0.03(1) and thus thestereochemistry of the structures depicted here are well established andare consistent with the purported stereochemistry for the compound:

Crystallographic co-ordinates and other relevant data are tabulated inthe form of a SHELX file in Table 17.

The conformational disorder can be represented (in first approximation)by the “thermal ellipsoids” of the atomic positions, as presented onFIG. 19. It can be seen that the major regions of disorder lie in themethyl groups and in the besylate.

The difference between the two independent molecules comes mainly fromthe ester chains as seen in FIG. 20. One molecule has the ester chainbeing coplanar with the imidazole ring, whereas the other molecule hasthe ester chain being orthogonal.

The conformation of the ester chains are different to that adopted inForm 2 (FIG. 21). The orthogonal conformation observed in Form 1 bearsthe greatest similarity to that found in Form 2.

The two independent besylates have staggered conformations (FIG. 22). Nosubstantial differences in bond lengths are apparent.

One besylate adopts the conformation observed for the besylate in Form 2(FIG. 23).

The resolved crystal structure, viewed along the crystallographic a, band c axes, is illustrated in FIGS. 24a, b and c respectively. FIG. 25summarises the shortest contacts observed in the crystal packing.

Each compound interacts with the two independent besylates. Inparticular, a short distance (hydrogen-bond type) is established betweenone oxygen atom of one besylate and the protonated nitrogen of theimidazole ring of the compound. The second independent compoundinteracts similarly, but with the second independent besylate.

Other close contacts (C—O, H—O) are observed between the compounds andthe besylates mainly in the vicinity of the imidazole and pyridyl ring.Some close contacts are also observed between the two compoundsthemselves (Br—N, C—C, O—H) and the two besylate themselves (O—Hcontacts) but to a lesser extent for the latter.

Using the crystal structure determined experimentally, a powderdiffraction pattern for Form 1 has been calculated usingCrystalDiffract® (CrystalDiffract is a registered TradeMark ofCrystalMaker Ltd) and is depicted in FIG. 26. This powder patternmatches the experimental powder pattern reported for Form 1.

Example 10

Crystal Structure of Form 2

A crystal of compound of formula (I) besylate Form 2, which has a platehabit, is imaged in FIG. 27.

A single plate habit crystal (ca. 0.7×0.30×0.25 mm in size) was selectedand its cell parameters determined at 260K then at 190K. No transitionwas observed on lowering the temperature between 260-190K. The structureanalysed here is for the data at 190K; parameters of the crystal and theX-ray diffraction refinement are given in Table 16.

TABLE 16 Data of the ethanol:ethyl acetate grown crystal of compound offormula (I) besylate, Form 2. Crystal State Code CNS7056 besylateSolvent ethanol Anti-solvent/Co-solvent ethyl acetate Crystal Morphologyplate Crystal Size (mm) 0.7 × 0.30 × 0.25 Colour colourless CrystalStructure Formula C₂₇H₂₅Br₁N₄O₅S₁ Formula Weight 597.49 SystemOrthorhombic Space Group P 2₁2₁2₁ Unit Cell a (Å)  8.92130(10) b (Å)11.1526(2) c (Å) 25.8345(4) α (°) 90 β (°) 90 γ (°) 90 Volume (Å³)2570.65(7) Z (No. molecules in unit) 4 Z′ (No. molecules in asymmetric 1unit) Density (g cm³) 1.544 Absorption μ [MoKα] (mm⁻¹) 1.727 F(000) 1224Data Collection Temperature, (K) 190 Instrument Kappa CCD diffractometerScan Type ω Absorption Correction Type multi-scan No. of MeasuredReflections 5750 No. of Independent Reflections 5727 θ min/max (°) 5.15/27.48 h min/max −11/11 k min/max −14/14 l min/max −33/33Refinement Refinement On F I/σ(I) Cut-off 3 No. of Used Reflections 4067No. of Parameters 344 R factor (%) 3.85 Rw factor (%) 3.66 S 1.12Δρ(min) Å⁻³ −0.6 Δρ(max) Å⁻³ 0.5 Max Shift/Error 0.0003 Flack Parameter 0.011(9)

The content of the asymmetric unit is displayed in FIG. 28. It consistsof one independent molecule of the compound and one independentbesylate. The compound has the imidazole-Nitrogen protonated.

The Flack “Enantiopole” parameter was determined as 0.011(9) and thusthe stereochemistry of the structures depicted here are well establishedand are consistent with the purported stereochemistry for the compound.Crystallographic co-ordinates and other relevant data are tabulated inthe form of a SHELX file in Table 18.

The conformational disorder can be represented (in first approximation)by the “thermal ellipsoids” of the atomic positions, as presented onFIG. 29. It can be seen that the major regions of disorder lie in thebesylate.

As discussed above, the conformation of the ester chain in Form 2,depicted in FIG. 30, is different to that adopted in Form 1.

However, the conformation of the besylate is similar to the one observedfor one of the besylate in Form 1 (FIG. 31).

The resolved crystal structure, viewed along the crystallographic a, band c axes, is illustrated in FIGS. 32a, b and c respectively with FIG.33 summarising the shortest contacts observed in the crystal packing.The compound establishes a short contact (hydrogen-bond type) with oneoxygen atom of the besylate through its protonated nitrogen of theimidazole ring. Other short contacts (C—C, C—O, H—O) are observedbetween the compound and the besylate through the imidazole ring.

Some close contacts are also observed between the two compoundsthemselves (Br—C, C—C, O—C, O—H), most of which are via the ester chain.There are no close contacts between the besylate themselves.

Using the crystal structure determined experimentally, a powderdiffraction pattern for Form 2 has been calculated usingCrystalDiffract® (FIG. 34). This powder pattern matches the experimentalpowder pattern reported for Form 2.

TABLE 17 Crystallographic co-ordinates and other relevant data tabulatedin the form of a SHELX File for Compound of formula (I) besylate Form 1.TITL 12161316 Compound CNS7056 Form 1 CELL 0.71073 7.687 29.261 12.37690.000 97.788 90.000 ZERR 2 0.0001 0.0005 0.0003 0.0000 0.0008 0.0000LATT −1 SYMM −X, Y + 0.500, −Z SFAC C 2.3100 20.8439 1.0200 10.20751.5886 0.5687 0.8650 = 51.6512 0.2156 0.0033 0.0016 1.15 0.7700 12.0110SFAC H 0.4930 10.5109 0.3229 26.1257 0.1402 3.1424 0.0408 = 57.79980.0030 0.0000 0.0000 0.06 0.3200 1.0079 SFAC O 3.0485 13.2771 2.28685.7011 1.5463 0.3239 0.8670 = 32.9089 0.2508 0.0106 0.0060 3.25 0.770015.9994 SFAC BR 17.1789 2.1723 5.2358 16.5796 5.6377 0.2609 3.9851 =41.4328 2.9557 −0.2901 2.4595 1000.00 1.1000 79.9040 SFAC N 12.21260.0057 3.1322 9.8933 2.0125 28.9975 1.1663 = 0.5826 −11.5290 0.00610.0033 1.96 0.7700 14.0067 SFAC S 6.9053 1.4679 5.2034 22.2151 1.43790.2536 1.5863 = 56.1720 0.8669 0.1246 0.1234 53.20 1.1100 32.0660 UNIT108. 100. 20. 4. 16. 4. S80 6 0.23964 0.43139 0.09908 11.00000 0.046340.03299 = 0.04052 0.00002 0.01880 −0.00340 O81 3 0.16028 0.39374 0.1514311.00000 0.06864 0.04111 = 0.05255 −0.00210 0.02801 0.00002 O82 30.14598 0.47435 0.11207 11.00000 0.08099 0.03603 = 0.04614 0.005450.03373 −0.00236 O83 3 0.42589 0.43401 0.12925 11.00000 0.05754 0.08564= 0.05198 −0.01536 0.01792 −0.00644 C84 1 0.20581 0.41866 −0.0432411.00000 0.05949 0.04444 = 0.02903 0.00359 0.01728 0.00704 C85 1 0.036240.41100 −0.09142 11.00000 0.06649 0.10092 = 0.05586 0.01088 0.017510.00507 C86 1 0.00323 0.39810 −0.20187 11.00000 0.08670 0.14765 =−0.02096 −0.03160 −0.00004 C87 1 0.14311 0.39209 −0.25693 11.000000.07916 0.11651 = 0.06238 −0.01696 0.00195 0.02481 C88 1 0.30473 0.39806−0.20987 11.00000 0.09246 0.09710 = 0.04155 0.00157 0.01795 0.02685 C891 0.33456 0.41126 −0.10133 11.00000 0.05999 0.09817 = 0.07178 −0.014510.00886 0.02173 S90 6 0.68868 0.81145 0.51625 11.00000 0.04072 0.02869 =0.05437 0.00158 0.00214 0.00223 O91 3 0.79129 0.77464 0.57315 11.000000.08025 0.03751 = 0.04867 −0.00213 −0.00954 0.01626 O92 3 0.526010.81933 0.56122 11.00000 0.04778 0.05360 = 0.06934 −0.00642 0.017020.00039 O93 3 0.78935 0.85213 0.50763 11.00000 0.07515 0.04369 = 0.05025−0.01354 0.01764 −0.01547 C94 1 0.62446 0.78970 0.38130 11.00000 0.042320.04028 = 0.05049 0.00898 0.00929 0.00525 C95 1 0.74659 0.76959 0.3239611.00000 0.06194 0.06998 = 0.03238 0.00341 −0.00103 0.00990 C96 10.69911 0.75023 0.22476 11.00000 0.12417 0.10337 = 0.03441 0.015370.02421 0.03314 C97 1 0.51941 0.75295 0.17732 11.00000 0.11897 0.11939 =−0.01324 −0.00963 −0.00586 C98 1 0.40301 0.77268 0.23169 11.000000.06106 0.10242 = 0.00570 −0.01263 −0.00283 C99 1 0.45446 0.791930.33547 11.00000 0.05307 0.07089 = 0.00728 −0.00426 −0.01944 BR1 40.06011 0.52462 0.55140 11.00000 0.04153 0.05204 = 0.07369 −0.005240.02434 0.00670 C2 1 0.25757 0.50395 0.49005 11.00000 0.02832 0.04536 =0.03350 −0.00752 0.01511 0.00763 C3 1 0.28921 0.45781 0.47911 11.000000.03135 0.03107 = 0.04579 0.00145 0.00221 −0.00479 C4 1 0.42954 0.443930.43174 11.00000 0.03767 0.03461 = −0.00320 −0.00151 −0.00125 C5 10.54674 0.47556 0.39943 11.00000 0.03535 0.02939 = 0.03479 −0.003900.00647 0.00183 C6 1 0.51907 0.52242 0.41134 11.00000 0.04226 0.03479 =0.04333 −0.00172 0.00236 0.00188 C7 1 0.37213 0.53602 0.45794 11.000000.03598 0.02793 = 0.04586 −0.00044 0.01652 0.00336 C8 1 0.64321 0.558240.38118 11.00000 0.03964 0.02453 = 0.02719 0.00516 0.00457 0.00373 C9 10.68998 0.59645 0.46059 11.00000 0.03743 0.03694 = 0.04454 −0.003750.01588 0.00649 N10 5 0.69097 0.58514 0.56581 11.00000 0.06070 0.03116 =0.04918 −0.00640 0.02020 −0.00054 C11 1 0.74090 0.61847 0.63822 11.000000.06804 0.05787 = 0.04752 −0.00600 0.01695 −0.00669 C12 1 0.785150.66221 0.61053 11.00000 0.05480 0.04458 = 0.05526 −0.02125 0.01554−0.00787 C13 1 0.77550 0.67229 0.50132 11.00000 0.04463 0.03102 =0.05452 0.00407 0.01432 −0.00038 C14 1 0.73186 0.63955 0.42553 11.000000.04272 0.03021 = 0.04282 −0.00243 0.01499 0.00270 N15 5 0.71451 0.559720.29408 11.00000 0.04979 0.02502 = 0.03692 0.00975 0.01748 0.00775 C16 10.67500 0.52204 0.21324 11.00000 0.04463 0.02346 = 0.04948 −0.004640.01738 0.00561 C17 1 0.75857 0.47996 0.26673 11.00000 0.04549 0.02673 =0.01954 −0.00693 0.00506 −0.00121 N18 5 0.70009 0.45973 0.35317 11.000000.03293 0.02806 = 0.02597 −0.00088 0.00321 0.00207 C19 1 0.81334 0.424090.39181 11.00000 0.03678 0.02848 = 0.03351 −0.00426 0.00585 0.00488 C201 0.93968 0.42402 0.32661 11.00000 0.03371 0.02802 = 0.03711 0.002020.00106 0.00680 N21 5 0.90585 0.45925 0.25315 11.00000 0.04775 0.03416 =0.02231 −0.01051 0.01052 −0.00308 C22 1 0.79597 0.39511 0.48941 11.000000.03997 0.03711 = 0.04548 0.01039 0.00508 0.00197 C23 1 0.74788 0.534070.10940 11.00000 0.05650 0.04712 = 0.03514 0.00836 0.00449 0.00605 C24 10.68780 0.50047 0.01647 11.00000 0.08242 0.04077 = 0.03001 −0.000460.01385 0.00523 C25 1 0.71419 0.51690 −0.09234 11.00000 0.06429 0.06543= 0.03392 0.00018 0.00559 −0.00499 O26 3 0.76261 0.55440 −0.1145011.00000 0.12347 0.08282 = 0.04188 0.01501 0.01658 −0.04001 O27 30.65910 0.48459 −0.16756 11.00000 0.10340 0.06919 = 0.03191 0.002530.01824 −0.00449 C28 1 0.66642 0.49760 −0.27953 11.00000 0.19131 0.12699= 0.01390 −0.01417 0.02134 −0.05279 BR51 4 1.06737 0.71057 0.9874311.00000 0.03812 0.08781 = 0.06774 0.00566 −0.00531 0.00447 C52 10.84276 0.73306 0.93243 11.00000 0.03132 0.05952 = 0.03819 0.003580.00226 −0.00263 C53 1 0.81293 0.77906 0.93249 11.00000 0.04627 0.06820= 0.03723 −0.00581 0.00481 −0.00474 C54 1 0.65043 0.79579 0.8826911.00000 0.04551 0.03939 = 0.04858 −0.00084 0.00376 −0.01071 C55 10.51946 0.76552 0.84226 11.00000 0.04294 0.03573 = 0.03413 0.000620.00952 −0.00208 C56 1 0.54512 0.71765 0.84581 11.00000 0.02688 0.03659= 0.04586 −0.00025 0.00561 0.00047 C57 1 0.71139 0.70186 0.8891411.00000 0.03105 0.04840 = 0.04447 −0.00668 −0.00429 0.00504 C58 10.40956 0.68443 0.79765 11.00000 0.03348 0.02893 = 0.04334 0.000700.00351 0.00421 C59 1 0.38048 0.64253 0.86694 11.00000 0.03165 0.03488 =0.04951 0.00002 0.00425 0.00528 N60 5 0.42879 0.64650 0.97247 11.000000.03542 0.05694 = 0.03178 0.00872 0.00154 0.00467 C61 1 0.38962 0.610261.03529 11.00000 0.04457 0.06338 = 0.05765 0.01416 0.00707 0.00171 C62 10.30187 0.57202 0.98967 11.00000 0.06548 0.04957 = 0.11303 0.034560.03582 0.00696 C63 1 0.25733 0.56863 0.88018 11.00000 0.07395 0.04664 =0.09803 0.00115 0.01240 −0.01007 C64 1 0.29561 0.60475 0.81590 11.000000.08355 0.04152 = 0.05459 −0.00010 0.00128 −0.02308 N65 5 0.313440.68797 0.70771 11.00000 0.03846 0.03072 = 0.04952 −0.00160 0.000320.00597 C66 1 0.33129 0.72953 0.64125 11.00000 0.03574 0.02676 = 0.055190.00406 0.00580 0.00330 C67 1 0.26347 0.76733 0.70231 11.00000 0.038030.03316 = 0.04166 0.01528 0.00868 0.00029 N68 5 0.35122 0.78274 0.7976411.00000 0.03387 0.03259 = 0.05055 0.00549 0.00427 0.00218 C69 1 0.247630.81583 0.84108 11.00000 0.05345 0.03305 = 0.04570 0.00005 0.02067−0.00546 C70 1 0.09873 0.81841 0.77077 11.00000 0.04465 0.03799 =0.06107 0.00794 0.01464 0.00936 N71 5 0.10819 0.78841 0.68720 11.000000.03892 0.03266 = 0.05306 0.00974 0.01063 0.00803 C72 1 0.30218 0.840640.94469 11.00000 0.08091 0.04934 = 0.08052 −0.01505 0.02392 −0.00661 C731 0.22541 0.72388 0.52948 11.00000 0.04039 0.05583 = 0.03295 0.000470.00724 −0.00165 C74 1 0.30154 0.68566 0.46508 11.00000 0.05896 0.05343= 0.05504 −0.00576 0.00667 0.02016 C75 1 0.18003 0.67204 0.3658711.00000 0.05296 0.05447 = 0.04241 0.00546 0.01355 0.00171 O76 3 0.067820.69497 0.31818 11.00000 0.05552 0.07543 = 0.05719 −0.00702 −0.001940.02108 O77 3 0.22119 0.62976 0.33149 11.00000 0.08466 0.04267 = 0.04376−0.00714 0.00726 0.00488 C78 1 0.10717 0.61220 0.23887 11.00000 0.063020.09312 = 0.07465 −0.02449 0.02418 −0.00980 H611 2 10.42342 10.6111111.10933 11.00000 0.06582 H621 2 10.27371 10.54835 11.03412 11.000000.09086 H631 2 10.20282 10.54235 10.84949 11.00000 0.08585 H641 210.26600 10.60396 10.74163 11.00000 0.07058 H661 2 10.45616 10.7349410.63683 11.00000 0.04658 H701 2 10.00528 10.83765 10.77749 11.000000.05724 H721 2 10.20390 10.85662 10.96784 11.00000 0.10482 H722 210.39143 10.86250 10.93477 11.00000 0.10500 H723 2 10.34863 10.8197511.00178 11.00000 0.10479 H731 2 10.22647 10.75279 10.49048 11.000000.05050 H732 2 10.10462 10.71635 10.53573 11.00000 0.05107 H741 210.41143 10.69632 10.44327 11.00000 0.06599 H742 2 10.32279 10.6590510.51273 11.00000 0.06616 H571 2 10.73613 10.67093 10.88928 11.000000.04893 H531 2 10.89874 10.79871 10.96543 11.00000 0.05990 H541 210.63029 10.82681 10.87790 11.00000 0.05285 H161 2 10.54702 10.5173110.19609 11.00000 0.04687 H201 2 11.03302 10.40374 10.33036 11.000000.03977 H221 2 10.90306 10.37871 10.51025 11.00000 0.06107 H222 210.77354 10.41394 10.54853 11.00000 0.06102 H223 2 10.70245 10.3737010.47387 11.00000 0.06087 H231 2 10.71028 10.56434 10.08666 11.000000.05487 H232 2 10.87494 10.53365 10.12431 11.00000 0.05471 H241 210.56546 10.49241 10.01723 11.00000 0.06095 H242 2 10.75795 10.4732310.02815 11.00000 0.06099 H111 2 10.74728 10.61186 10.71244 11.000000.06882 H121 2 10.81997 10.68398 10.66349 11.00000 0.06182 H131 210.79812 10.70154 10.48020 11.00000 0.05215 H141 2 10.72939 10.6454410.35226 11.00000 0.04595 H71 2 10.35042 10.56684 10.46668 11.000000.04408 H31 2 10.21444 10.43638 10.50355 11.00000 0.04223 H41 2 10.4493110.41280 10.42055 11.00000 0.04056 H891 2 10.44977 10.41481 9.9322611.00000 0.09285 H881 2 10.39917 10.39332 9.75106 11.00000 0.09266 H8712 10.12372 10.38356 9.66972 11.00000 0.10194 H861 2 9.88808 10.393889.76390 11.00000 0.11607 H851 2 9.94416 10.41466 9.94909 11.000000.08904 H951 2 10.86472 10.76918 10.35546 11.00000 0.06580 H961 210.78321 10.73544 10.18942 11.00000 0.10497 H971 2 10.48493 10.7405510.10914 11.00000 0.10604 H981 2 10.28646 10.77378 10.20054 11.000000.08719 H991 2 10.37377 10.80653 10.37249 11.00000 0.07037 H781 210.14480 10.58182 10.22240 11.00000 0.11588 H782 2 10.11102 10.6319710.17669 11.00000 0.11581 H783 2 9.98883 10.61082 10.25546 11.000000.11600 H711 2 10.01359 10.78308 10.62464 11.00000 0.05205 H211 210.98261 10.46785 10.19729 11.00000 0.04161 H281 2 10.62358 10.471809.67092 11.00000 0.11566 H282 2 10.59036 10.52501 9.70225 11.000000.11566 H283 2 10.79029 10.50514 9.71088 11.00000 0.11566

TABLE 18 Crystallographic co-ordinates and other relevant data tabulatedin the form of a SHELX File for Compound of formula (I) besylate Form 2.TITL 1142055 Compound CNS7056 form 2 CELL 0.71073 8.921 11.154 25.83490.000 90.000 90.000 ZERR 4 0.0001 0.0002 0.0004 0.0000 0.0000 0.0000LATT −1 SYMM X + 0.500, −Y + 0.500, −Z SYMM −X, Y + 0.500, −Z + 0.500SYMM −X + 0.500, −Y, Z + 0.500 SFAC C 2.3100 20.8439 1.0200 10.20751.5886 0.5687 0.8650 = 51.6512 0.2156 0.0033 0.0016 1.15 0.7700 12.0110SFAC H 0.4930 10.5109 0.3229 26.1257 0.1402 3.1424 0.0408 = 57.79980.0030 0.0000 0.0000 0.06 0.3200 1.0079 SFAC BR 17.1789 2.1723 5.235816.5796 5.6377 0.2609 3.9851 = 41.4328 2.9557 −0.2901 2.4595 1000.001.1000 79.9040 SFAC N 12.2126 0.0057 3.1322 9.8933 2.0125 28.9975 1.1663= 0.5826 −11.5290 0.0061 0.0033 1.96 0.7700 14.0067 SFAC O 3.048513.2771 2.2868 5.7011 1.5463 0.3239 0.8670 = 32.9089 0.2508 0.01060.0060 3.25 0.7700 15.9994 SFAC S 6.9053 1.4679 5.2034 22.2151 1.43790.2536 1.5863 = 56.1720 0.8669 0.1246 0.1234 53.20 1.1100 32.0660 UNIT108. 100. 4. 16. 20. 4. BR1 3 −0.04819 −0.10880 −0.27710 11.000000.07032 0.03277 = 0.00144 −0.01238 −0.02224 C2 1 −0.15018 −0.21830−0.32054 11.00000 0.02777 0.02177 = −0.00009 −0.00209 −0.00471 C3 1−0.17401 −0.18875 −0.37205 11.00000 0.02963 0.01861 = 0.02702 0.006230.00188 −0.00107 C4 1 −0.24491 −0.26965 −0.40362 11.00000 0.028250.02442 = 0.01718 0.00327 0.00106 −0.00145 C5 1 −0.29275 −0.37943−0.38401 11.00000 0.02223 0.01822 = 0.01875 −0.00067 0.00141 0.00066 C61 −0.27139 −0.40894 −0.33163 11.00000 0.02028 0.01967 = 0.01926 0.001820.00105 −0.00153 C7 1 −0.20042 −0.32532 −0.29979 11.00000 0.028090.02763 = 0.01685 0.00206 0.00190 −0.00055 C8 1 −0.32197 −0.52600−0.30927 11.00000 0.01670 0.02233 = 0.00135 −0.00476 −0.00144 C9 1−0.39853 −0.52353 −0.25770 11.00000 0.01623 0.02317 = 0.00259 −0.00384−0.00281 N10 4 −0.46099 −0.41943 −0.24363 11.00000 0.02251 0.02613 =0.02353 −0.00189 0.00408 0.00155 C11 1 −0.52777 −0.41652 −0.1969711.00000 0.02617 0.03441 = 0.02357 −0.00451 0.00365 0.00346 C12 1−0.53610 −0.51390 −0.16425 11.00000 0.02740 0.04329 = 0.02040 −0.003350.00652 −0.00779 C13 1 −0.47518 −0.62062 −0.17997 11.00000 0.035840.03200 = 0.02405 0.00767 0.00645 −0.00687 C14 1 −0.40334 −0.62685−0.22730 11.00000 0.02879 0.02223 = 0.02565 0.00090 0.00272 −0.00057 N154 −0.30040 −0.62781 −0.33049 11.00000 0.02151 0.02416 = 0.01713 0.00287−0.00002 0.00182 C16 1 −0.21928 −0.62991 −0.38036 11.00000 0.023300.02286 = 0.01602 0.00057 0.00417 0.00450 C17 1 −0.32510 −0.57975−0.41920 11.00000 0.02824 0.02308 = 0.01704 −0.00121 0.00336 −0.00285N18 4 −0.36294 −0.46298 −0.41818 11.00000 0.02482 0.02037 = 0.014830.00150 −0.00070 0.00079 C19 1 −0.46920 −0.44117 −0.45641 11.000000.03022 0.02725 = 0.01634 0.00325 0.00039 −0.00224 C20 1 −0.49445−0.54753 −0.47911 11.00000 0.03071 0.03401 = 0.00110 −0.00174 −0.00215N21 4 −0.40440 −0.63226 −0.45591 11.00000 0.03619 0.02354 = 0.02146−0.00463 0.00147 −0.00154 C22 1 −0.54310 −0.32298 −0.46595 11.000000.03636 0.03429 = 0.00778 −0.00982 −0.00011 C23 1 −0.15995 −0.75547−0.39193 11.00000 0.03430 0.02640 = 0.01793 −0.00359 0.00177 0.00554 C241 −0.06166 −0.79435 −0.34621 11.00000 0.04707 0.03881 = 0.02350 0.000410.00034 0.01530 C25 1 0.06625 −0.87542 −0.35603 11.00000 0.03182 0.02650= 0.00340 −0.00125 −0.00016 O26 5 0.17233 −0.88334 −0.32760 11.000000.03778 0.06570 = 0.03313 −0.01160 −0.01173 0.00417 O27 5 0.05245−0.94265 −0.39885 11.00000 0.03130 0.03874 = 0.02467 −0.00799 −0.003300.01418 C28 1 0.17574 −1.02443 −0.40865 11.00000 0.05622 0.08123 =0.03697 −0.01153 −0.00496 0.04396 S80 6 −0.94275 −0.52899 −0.4962411.00000 0.03340 0.02679 = 0.02442 0.00000 0.00210 −0.00075 O81 5−0.83867 −0.47114 −0.53020 11.00000 0.05118 0.08336 = 0.02297 −0.00622−0.02476 O82 5 −1.08156 −0.46260 −0.49186 11.00000 0.04015 0.07788 =0.05503 −0.01022 −0.00539 0.01721 O83 5 −0.97025 −0.65272 −0.5072611.00000 0.13945 0.03230 = 0.06071 −0.01467 0.01447 −0.00725 C84 1−0.86288 −0.52210 −0.43343 11.00000 0.02735 0.05893 = 0.02832 0.015090.00686 −0.00534 C85 1 −0.87781 −0.41462 −0.40588 11.00000 0.037630.08695 = 0.03855 −0.01799 0.00427 −0.00754 C86 1 −0.81420 −0.39965−0.35764 11.00000 0.05438 0.16315 = 0.04455 −0.02905 0.00147 −0.02905C87 1 −0.73766 −0.49241 −0.33773 11.00000 0.06202 0.20226 = 0.03510−0.02105 −0.05062 C88 1 −0.71885 −0.60444 −0.36221 11.00000 0.042170.17120 = 0.11388 0.10762 −0.01320 −0.03729 C89 1 −0.78500 −0.61610−0.41251 11.00000 0.03725 0.08786 = 0.05538 −0.00772 −0.01074 H891 29.22557 9.31210 9.56883 11.00000 0.08027 H881 2 9.33331 9.33306 9.6528911.00000 0.13097 H851 2 9.06867 9.64846 9.57936 11.00000 0.06577 H861 29.17563 9.67239 9.66111 11.00000 0.10509 H161 2 9.86530 9.42517 9.6224511.00000 0.02469 H111 2 9.42959 9.65626 9.81326 11.00000 0.03383 H121 29.41618 9.49292 9.86839 11.00000 0.03606 H131 2 9.51614 9.31066 9.8405911.00000 0.03697 H141 2 9.64103 9.30191 9.76144 11.00000 0.03108 H231 29.89972 9.24922 9.57680 11.00000 0.03066 H232 2 9.75764 9.18723 9.6037211.00000 0.03099 H241 2 9.87585 9.16237 9.67759 11.00000 0.04434 H242 29.97980 9.27746 9.67100 11.00000 0.04489 H281 2 10.15353 8.92912 9.5608511.00000 0.08666 H282 2 10.18989 8.92278 9.62053 11.00000 0.08723 H283 210.26566 9.02166 9.58620 11.00000 0.08710 H201 2 9.44027 9.43682 9.4945711.00000 0.03327 H221 2 9.36727 9.66624 9.51370 11.00000 0.05146 H222 29.52479 9.72860 9.51527 11.00000 0.05104 H223 2 9.43193 9.71611 9.5660111.00000 0.05131 H41 2 9.73983 9.74902 9.56204 11.00000 0.02807 H31 29.85823 9.88568 9.61518 11.00000 0.03001 H71 2 9.81367 9.65791 9.7349011.00000 0.02870 H871 2 9.30621 9.51762 9.69480 11.00000 0.13226 H211 29.59801 9.29339 9.53630 11.00000 0.03270

TABLE 19 Bond lengths for Compound of formula (I) besylate Form 1. S80O81 1.454(5) Å S80 O82 1.468(5) Å S80 O83 1.432(6) Å S80 C84 1.784(7) ÅC84 C85 1.376(12) Å C84 C89 1.318(12) Å C85 C86 1.408(14) Å C85 H8510.927 Å C86 C87 1.360(16) Å C86 H861 0.936 Å C87 C88 1.310(15) Å C87H871 0.934 Å C88 C89 1.386(14) Å C88 H881 0.935 Å C89 H891 0.932 Å S90O91 1.459(5) Å S90 O92 1.454(6) Å S90 O93 1.431(5) Å S90 C94 1.793(8) ÅC94 C95 1.383(11) Å C94 C99 1.354(11) Å C95 C96 1.356(13) Å C95 H9510.938 Å C96 C97 1.428(17) Å C96 H961 0.934 Å C97 C98 1.323(15) Å C97H971 0.924 Å C98 C99 1.409(13) Å C98 H981 0.927 Å C99 H991 0.924 Å Br1C2 1.886(6) Å C2 C3 1.382(9) Å C2 C7 1.381(9) Å C3 C4 1.358(10) Å C3 H310.928 Å C4 C5 1.388(9) Å C4 H41 0.937 Å C5 C6 1.398(9) Å C5 N18 1.454(8)Å C6 C7 1.394(9) Å C6 C8 1.498(9) Å C7 H71 0.926 Å C8 C9 1.500(9) Å C8N15 1.274(8) Å C9 N10 1.343(9) Å C9 C14 1.386(9) Å N10 C11 1.345(10) ÅC11 C12 1.379(11) Å C11 H111 0.933 Å C12 C13 1.375(11) Å C12 H121 0.927Å C13 C14 1.351(10) Å C13 H131 0.918 Å C14 H141 0.921 Å N15 C16 1.492(9)Å C16 C17 1.500(9) Å C16 C23 1.511(9) Å C16 H161 0.988 Å C17 N181.352(8) Å C17 N21 1.315(8) Å N18 C19 1.400(8) Å C19 C20 1.344(9) Å C19C22 1.496(9) Å C20 N21 1.376(8) Å C20 H201 0.927 Å N21 H211 1.000 Å C22H221 0.958 Å C22 H222 0.950 Å C22 H223 0.953 Å C23 C24 1.536(11) Å C23H231 0.962 Å C23 H232 0.969 Å C24 C25 1.470(11) Å C24 H241 0.971 Å C24H242 0.962 Å C25 O26 1.202(10) Å C25 O27 1.354(10) Å O27 C28 1.445(10) ÅC28 H281 1.000 Å C28 H282 1.000 Å C28 H283 1.000 Å Br51 C52 1.886(7) ÅC52 C53 1.366(11) Å C52 C57 1.412(10) Å C53 C54 1.404(11) Å C53 H5310.927 Å C54 C55 1.383(10) Å C54 H541 0.921 Å C55 C56 1.414(9) Å C55 N681.427(9) Å C56 C57 1.396(9) Å C56 C58 1.489(9) Å C57 H571 0.925 Å C58C59 1.530(10) Å C58 N65 1.254(8) Å C59 N60 1.314(9) Å C59 C64 1.391(10)Å N60 C61 1.372(10) Å C61 C62 1.386(14) Å C61 H611 0.918 Å C62 C631.355(15) Å C62 H621 0.928 Å C63 C64 1.378(13) Å C63 H631 0.932 Å C64H641 0.917 Å N65 C66 1.485(8) Å C66 C67 1.474(9) Å C66 C73 1.516(10) ÅC66 H661 0.982 Å C67 N68 1.354(9) Å C67 N71 1.334(8) Å N68 C69 1.406(9)Å C69 C70 1.343(11) Å C69 C72 1.484(12) Å C70 N71 1.366(10) Å C70 H7010.925 Å N71 H711 1.000 Å C72 H721 0.964 Å C72 H722 0.958 Å C72 H7230.965 Å C73 C74 1.535(10) Å C73 H731 0.975 Å C73 H732 0.967 Å C74 C751.493(12) Å C74 H741 0.972 Å C74 H742 0.977 Å C75 O76 1.185(9) Å C75 O771.360(9) Å O77 C78 1.440(11) Å C78 H781 0.965 Å C78 H782 0.966 Å C78H783 0.960 Å

TABLE 20 Angles for Compound of formula (I) besylate Form 1 O81 S80 O82111.0(3)° O81 S80 O83 112.9(4)° O82 S80 O83 114.4(4)° O81 S80 C84105.5(3)° O82 S80 C84 106.2(3)° O83 S80 C84 106.0(4)° S80 C84 C85117.7(6)° S80 C84 C89 123.6(7)° C85 C84 C89 118.3(8)° C84 C85 C86120.0(9)° C84 C85 H851 119.626° C86 C85 H851 120.377° C85 C86 C87118.1(10)° C85 C86 H861 120.636° C87 C86 H861 121.303° C86 C87 C88121.8(10)° C86 C87 H871 119.251° C88 C87 H871 118.984° C87 C88 C89119.3(10)° C87 C88 H881 120.392° C89 C88 H881 120.264° C84 C89 C88122.5(10)° C84 C89 H891 118.485° C88 C89 H891 119.061° O91 S90 O92111.7(3)° O91 S90 O93 112.8(4)° O92 S90 O93 113.5(3)° O91 S90 C94104.5(3)° O92 S90 C94 105.7(3)° O93 S90 C94 108.0(3)° S90 C94 C95120.6(6)° S90 C94 C99 120.1(6)° C95 C94 C99 119.3(8)° C94 C95 C96121.6(9)° C94 C95 H951 118.566° C96 C95 H951 119.820° C95 C96 C97118.4(10)° C95 C96 H961 119.911° C97 C96 H961 121.695° C96 C97 C98119.9(8)° C96 C97 H971 119.699° C98 C97 H971 120.397° C97 C98 C99120.8(9)° C97 C98 H981 119.080° C99 C98 H981 120.094° C94 C99 C98119.9(9)° C94 C99 H991 119.276° C98 C99 H991 120.819° Br1 C2 C3121.0(5)° Br1 C2 C7 118.5(5)° C3 C2 C7 120.5(5)° C2 C3 C4 119.7(6)° C2C3 H31 120.203° C4 C3 H31 120.109° C3 C4 C5 120.6(6)° C3 C4 H41 120.600°C5 C4 H41 118.766° C4 C5 C6 120.6(6)° C4 C5 N18 119.6(5)° C6 C5 N18119.8(6)° C5 C6 C7 117.8(6)° C5 C6 C8 123.3(6)° C7 C6 C8 118.8(6)° C2 C7C6 120.6(6)° C2 C7 H71 119.721° C6 C7 H71 119.679° C6 C8 C9 117.5(5)° C6C8 N15 126.6(6)° C9 C8 N15 115.9(6)° C8 C9 N10 114.9(6)° C8 C9 C14121.2(6)° N10 C9 C14 123.9(6)° C9 N10 C11 115.5(6)° N10 C11 C12124.4(7)° N10 C11 H111 118.526° C12 C11 H111 117.061° C11 C12 C13117.4(7)° C11 C12 H121 121.279° C13 C12 H121 121.289° C12 C13 C14120.4(6)° C12 C13 H131 119.499° C14 C13 H131 120.125° C9 C14 C13118.3(6)° C9 C14 H141 120.274° C13 C14 H141 121.419° C8 N15 C16118.0(5)° N15 C16 C17 105.9(5)° N15 C16 C23 109.4(5)° C17 C16 C23112.4(5)° N15 C16 H161 110.723° C17 C16 H161 109.539° C23 C16 H161108.851° C16 C17 N18 122.7(6)° C16 C17 N21 130.3(6)° N18 C17 N21106.5(5)° C5 N18 C17 123.1(5)° C5 N18 C19 127.0(5)° C17 N18 C19109.8(5)° N18 C19 C20 105.2(5)° N18 C19 C22 125.3(6)° C20 C19 C22129.4(6)° C19 C20 N21 108.0(5)° C19 C20 H201 126.017° N21 C20 H201126.026° C17 N21 C20 110.5(5)° C17 N21 H211 124.840° C20 N21 H211124.681° C19 C22 H221 109.508° C19 C22 H222 109.778° H221 C22 H222108.808° C19 C22 H223 110.905° H221 C22 H223 108.786° H222 C22 H223109.018° C16 C23 C24 112.3(6)° C16 C23 H231 109.392° C24 C23 H231108.812° C16 C23 H232 108.378° C24 C23 H232 109.105° H231 C23 H232108.825° C23 C24 C25 114.3(7)° C23 C24 H241 109.968° C25 C24 H241110.030° C23 C24 H242 108.195° C25 C24 H242 105.346° H241 C24 H242108.752° C24 C25 O26 126.4(7)° C24 C25 O27 109.4(7)° O26 C25 O27123.9(7)° C25 O27 C28 115.2(7)° O27 C28 H281 109.674° O27 C28 H282109.261° H281 C28 H282 109.475° O27 C28 H283 109.465° H281 C28 H283109.476° H282 C28 H283 109.476° Br51 C52 C53 119.3(6)° Br51 C52 C57119.0(5)° C53 C52 C57 121.7(7)° C52 C53 C54 118.9(7)° C52 C53 H531120.141° C54 C53 H531 120.985° C53 C54 C55 119.8(7)° C53 C54 H541120.227° C55 C54 H541 120.000° C54 C55 C56 122.1(6)° C54 C55 N68119.4(6)° C56 C55 N68 118.5(6)° C55 C56 C57 117.2(6)° C55 C56 C58123.2(6)° C57 C56 C58 119.5(6)° C52 C57 C56 120.2(7)° C52 C57 H571119.709° C56 C57 H571 120.138° C56 C58 C59 116.5(6)° C56 C58 N65126.7(6)° C59 C58 N65 116.8(6)° C58 C59 N60 116.3(6)° C58 C59 C64118.5(7)° N60 C59 C64 125.0(7)° C59 N60 C61 116.1(7)° N60 C61 C62121.7(8)° N60 C61 H611 119.342° C62 C61 H611 118.993° C61 C62 C63120.6(8)° C61 C62 H621 120.029° C63 C62 H621 119.353° C62 C63 C64118.4(9)° C62 C63 H631 120.452° C64 C63 H631 121.124° C59 C64 C63118.1(8)° C59 C64 H641 120.844° C63 C64 H641 121.057° C58 N65 C66118.2(6)° N65 C66 C67 105.4(5)° N65 C66 C73 109.7(5)° C67 C66 C73111.5(6)° N65 C66 H661 109.122° C67 C66 H661 108.890° C73 C66 H661112.017° C66 C67 N68 121.8(6)° C66 C67 N71 130.3(7)° N68 C67 N71107.4(6)° C55 N68 C67 122.5(6)° C55 N68 C69 128.7(6)° C67 N68 C69108.7(6)° N68 C69 C70 105.5(6)° N68 C69 C72 124.0(7)° C70 C69 C72130.5(7)° C69 C70 N71 109.1(6)° C69 C70 H701 125.444° N71 C70 H701125.502° C67 N71 C70 109.2(6)° C67 N71 H711 125.400° C70 N71 H711125.366° C69 C72 H721 110.667° C69 C72 H722 109.838° H721 C72 H722108.539° C69 C72 H723 110.831° H721 C72 H723 108.455° H722 C72 H723108.445° C66 C73 C74 111.0(6)° C66 C73 H731 108.535° C74 C73 H731110.248° C66 C73 H732 110.751° C74 C73 H732 108.249° H731 C73 H732108.042° C73 C74 C75 112.4(6)° C73 C74 H741 108.496° C75 C74 H741109.125° C73 C74 H742 108.155° C75 C74 H742 108.578° H741 C74 H742110.035° C74 C75 O76 126.2(7)° C74 C75 O77 110.7(7)° O76 C75 O77123.0(7)° C75 O77 C78 115.6(7)° O77 C78 H781 109.214° O77 C78 H782109.848° H781 C78 H782 109.923° O77 C78 H783 109.687° H781 C78 H783109.026° H782 C78 H783 109.127°

TABLE 21 Bond Lengths for Compound of formula (I) besylate Form 2. Br1C2 1.892(3) Å C2 C3 1.387(5) Å C2 C7 1.383(5) Å C3 C4 1.371(5) Å C3 H310.938 Å C4 C5 1.392(5) Å C4 H41 0.921 Å C5 C6 1.406(4) Å C5 N18 1.428(4)Å C6 C7 1.395(5) Å C6 C8 1.497(4) Å C7 H71 0.924 Å C8 C9 1.497(4) Å C8N15 1.276(4) Å C9 N10 1.338(4) Å C9 C14 1.395(5) Å N10 C11 1.345(4) ÅC11 C12 1.378(5) Å C11 H111 0.935 Å C12 C13 1.370(5) Å C12 H121 0.948 ÅC13 C14 1.382(5) Å C13 H131 0.936 Å C14 H141 0.934 Å N15 C16 1.478(4) ÅC16 C17 1.487(5) Å C16 C23 1.527(5) Å C16 H161 0.976 Å C17 N18 1.346(4)Å C17 N21 1.320(4) Å N18 C19 1.391(4) Å C19 C20 1.342(5) Å C19 C221.494(5) Å C20 N21 1.378(5) Å C20 H201 0.912 Å N21 H211 0.854 Å C22 H2210.965 Å C22 H222 0.966 Å C22 H223 0.960 Å C23 C24 1.534(5) Å C23 H2310.969 Å C23 H232 0.981 Å C24 C25 1.478(5) Å C24 H241 0.960 Å C24 H2420.988 Å C25 O26 1.201(4) Å C25 O27 1.342(4) Å O27 C28 1.451(5) Å C28H281 0.964 Å C28 H282 0.965 Å C28 H283 0.962 Å S80 O81 1.431(3) Å S80O82 1.447(3) Å S80 O83 1.430(3) Å S80 C84 1.774(4) Å C84 C85 1.400(7) ÅC84 C89 1.369(7) Å C85 C86 1.380(7) Å C85 H851 0.932 Å C86 C87 1.342(13)Å C86 H861 0.943 Å C87 C88 1.410(13) Å C87 H871 0.934 Å C88 C891.433(10) Å C88 H881 0.925 Å C89 H891 0.940 Å

TABLE 22 Angles for Compound of formula (I) besylate Form 2. Br1 C2 C3119.3(3)° Br1 C2 C7 118.9(3)° C3 C2 C7 121.8(3)° C2 C3 C4 119.0(3)° C2C3 H31 120.033° C4 C3 H31 120.959° C3 C4 C5 120.3(3)° C3 C4 H41 119.485°C5 C4 H41 120.261° C4 C5 C6 121.0(3)° C4 C5 N18 118.9(3)° C6 C5 N18120.1(3)° C5 C6 C7 118.2(3)° C5 C6 C8 122.3(3)° C7 C6 C8 119.5(3)° C2 C7C6 119.7(3)° C2 C7 H71 120.432° C6 C7 H71 119.874° C6 C8 C9 117.7(3)° C6C8 N15 124.4(3)° C9 C8 N15 117.9(3)° C8 C9 N10 116.6(3)° C8 C9 C14120.0(3)° N10 C9 C14 123.4(3)° C9 N10 C11 116.7(3)° N10 C11 C12123.7(3)° N10 C11 H111 117.041° C12 C11 H111 119.278° C11 C12 C13118.8(3)° C11 C12 H121 120.443° C13 C12 H121 120.783° C12 C13 C14119.3(3)° C12 C13 H131 120.694° C14 C13 H131 119.952° C9 C14 C13118.1(3)° C9 C14 H141 120.942° C13 C14 H141 120.983° C8 N15 C16117.6(3)° N15 C16 C17 105.7(3)° N15 C16 C23 110.8(3)° C17 C16 C23115.7(3)° N15 C16 H161 107.681° C17 C16 H161 107.726° C23 C16 H161108.910° C16 C17 N18 120.7(3)° C16 C17 N21 131.2(3)° N18 C17 N21108.0(3)° C5 N18 C17 122.3(3)° C5 N18 C19 128.6(3)° C17 N18 C19109.0(3)° N18 C19 C20 105.7(3)° N18 C19 C22 124.9(3)° C20 C19 C22129.3(3)° C19 C20 N21 108.6(3)° C19 C20 H201 127.007° N21 C20 H201124.433° C17 N21 C20 108.7(3)° C17 N21 H211 125.926° C20 N21 H211125.351° C19 C22 H221 110.223° C19 C22 H222 109.368° H221 C22 H222108.664° C19 C22 H223 111.184° H221 C22 H223 109.452° H222 C22 H223107.885° C16 C23 C24 107.9(3)° C16 C23 H231 107.712° C24 C23 H231110.073° C16 C23 H232 111.123° C24 C23 H232 109.430° H231 C23 H232110.583° C23 C24 C25 118.8(3)° C23 C24 H241 107.661° C25 C24 H241104.516° C23 C24 H242 109.365° C25 C24 H242 106.503° H241 C24 H242109.671° C24 C25 O26 123.3(3)° C24 C25 O27 114.4(3)° O26 C25 O27122.4(3)° C25 O27 C28 115.2(3)° O27 C28 H281 108.952° O27 C28 H282110.269° H281 C28 H282 109.738° O27 C28 H283 108.681° H281 C28 H283110.225° H282 C28 H283 108.963° O81 S80 O82 111.9(2)° O81 S80 O83115.1(2)° O82 S80 O83 111.2(3)° O81 S80 C84 106.30(18)° O82 S80 C84104.5(2)° O83 S80 C84 107.0(2)° S80 C84 C85 117.6(4)° S80 C84 C89122.1(4)° C85 C84 C89 120.2(5)° C84 C85 C86 121.6(6)° C84 C85 H851119.148° C86 C85 H851 119.275° C85 C86 C87 117.5(8)° C85 C86 H861121.859° C87 C86 H861 120.606° C86 C87 C88 124.9(7)° C86 C87 H871117.763° C88 C87 H871 117.376° C87 C88 C89 116.0(7)° C87 C88 H881122.592° C89 C88 H881 121.435° C84 C89 C88 119.8(8)° C84 C89 H891120.080° C88 C89 H891 120.078°

What is claimed is:
 1. A pharmaceutical composition comprising a besylate salt of the compound of formula (I)

and at least one pharmaceutically acceptable carrier, excipient or diluent, wherein the pharmaceutical composition is an aqueous solution comprising dextrose or saline.
 2. The pharmaceutical composition according to claim 1, wherein the aqueous solution comprises saline.
 3. The pharmaceutical composition according to claim 1, wherein the aqueous solution comprises dextrose.
 4. A lyophilized composition comprising a besylate salt of the compound of formula (I)

and at least one pharmaceutically acceptable carrier, excipient or diluent, and dextrose or saline.
 5. An aqueous pharmaceutical composition comprising of the lyophilized composition of claim
 4. 6. The aqueous pharmaceutical composition according to claim 5, wherein the aqueous solution comprises saline.
 7. The aqueous pharmaceutical composition according to claim 5, wherein the aqueous solution comprises dextrose.
 8. A method of producing sedation in a subject, comprising administering to the subject an effective amount of a pharmaceutical composition comprising a besylate salt of the compound of formula (I)

and at least one pharmaceutically acceptable carrier, excipient or diluent, wherein the pharmaceutical composition is an aqueous solution comprising dextrose or saline.
 9. The method according to claim 8, wherein the aqueous solution comprises saline.
 10. The method according to claim 8, wherein the aqueous solution comprises dextrose. 